US20190274962A1 - Formulation of a micro drop pill and the preparation method thereof - Google Patents

Formulation of a micro drop pill and the preparation method thereof Download PDF

Info

Publication number
US20190274962A1
US20190274962A1 US16/422,857 US201916422857A US2019274962A1 US 20190274962 A1 US20190274962 A1 US 20190274962A1 US 201916422857 A US201916422857 A US 201916422857A US 2019274962 A1 US2019274962 A1 US 2019274962A1
Authority
US
United States
Prior art keywords
drop pill
dropping
temperature
micro
drying
Prior art date
Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
Granted
Application number
US16/422,857
Other versions
US11013694B2 (en
Inventor
Xijun Yan
Naifeng Wu
Kaijing Yan
Xiaobing Sun
Shunnan Zhang
Zhengliang Ye
Hai'ou Dong
Hongbo Zhang
Wensheng ZHANG
Lihong Zhou
Chenming Li
Cong Chen
Xiaofeng Liu
Shiqing Wang
Changsheng Rong
Yongfeng Zheng
Lijun FAN
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
Tasly Pharmaceutical Group Co Ltd
Original Assignee
Tasly Pharmaceutical Group Co Ltd
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
Filing date
Publication date
Priority claimed from CN201310291465.2A external-priority patent/CN104274416B/en
Priority claimed from CN201310290966.9A external-priority patent/CN104274319A/en
Priority claimed from CN201310290967.3A external-priority patent/CN104274517B/en
Application filed by Tasly Pharmaceutical Group Co Ltd filed Critical Tasly Pharmaceutical Group Co Ltd
Priority to US16/422,857 priority Critical patent/US11013694B2/en
Assigned to TASLY PHARMACEUTICAL GROUP CO., LTD. reassignment TASLY PHARMACEUTICAL GROUP CO., LTD. ASSIGNMENT OF ASSIGNORS INTEREST (SEE DOCUMENT FOR DETAILS). Assignors: CHEN, Cong, DONG, Hai'ou, FAN, LIJUN, LI, Chenming, LIU, XIAOFENG, RONG, Changsheng, SUN, XIAOBING, WANG, Shiqing, WU, NAIFENG, YAN, KAIJING, YAN, XIJUN, YE, ZHENGLIANG, ZHANG, HONGBO, ZHANG, SHUNNAN, ZHANG, WENSHENG, ZHENG, YONGFENG, ZHOU, LIHONG
Publication of US20190274962A1 publication Critical patent/US20190274962A1/en
Application granted granted Critical
Publication of US11013694B2 publication Critical patent/US11013694B2/en
Active legal-status Critical Current
Anticipated expiration legal-status Critical

Links

Classifications

    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61JCONTAINERS SPECIALLY ADAPTED FOR MEDICAL OR PHARMACEUTICAL PURPOSES; DEVICES OR METHODS SPECIALLY ADAPTED FOR BRINGING PHARMACEUTICAL PRODUCTS INTO PARTICULAR PHYSICAL OR ADMINISTERING FORMS; DEVICES FOR ADMINISTERING FOOD OR MEDICINES ORALLY; BABY COMFORTERS; DEVICES FOR RECEIVING SPITTLE
    • A61J3/00Devices or methods specially adapted for bringing pharmaceutical products into particular physical or administering forms
    • A61J3/06Devices or methods specially adapted for bringing pharmaceutical products into particular physical or administering forms into the form of pills, lozenges or dragees
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K36/00Medicinal preparations of undetermined constitution containing material from algae, lichens, fungi or plants, or derivatives thereof, e.g. traditional herbal medicines
    • A61K36/18Magnoliophyta (angiosperms)
    • A61K36/185Magnoliopsida (dicotyledons)
    • A61K36/25Araliaceae (Ginseng family), e.g. ivy, aralia, schefflera or tetrapanax
    • A61K36/258Panax (ginseng)
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K36/00Medicinal preparations of undetermined constitution containing material from algae, lichens, fungi or plants, or derivatives thereof, e.g. traditional herbal medicines
    • A61K36/18Magnoliophyta (angiosperms)
    • A61K36/185Magnoliopsida (dicotyledons)
    • A61K36/48Fabaceae or Leguminosae (Pea or Legume family); Caesalpiniaceae; Mimosaceae; Papilionaceae
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K36/00Medicinal preparations of undetermined constitution containing material from algae, lichens, fungi or plants, or derivatives thereof, e.g. traditional herbal medicines
    • A61K36/18Magnoliophyta (angiosperms)
    • A61K36/185Magnoliopsida (dicotyledons)
    • A61K36/48Fabaceae or Leguminosae (Pea or Legume family); Caesalpiniaceae; Mimosaceae; Papilionaceae
    • A61K36/481Astragalus (milkvetch)
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K36/00Medicinal preparations of undetermined constitution containing material from algae, lichens, fungi or plants, or derivatives thereof, e.g. traditional herbal medicines
    • A61K36/18Magnoliophyta (angiosperms)
    • A61K36/185Magnoliopsida (dicotyledons)
    • A61K36/53Lamiaceae or Labiatae (Mint family), e.g. thyme, rosemary or lavender
    • A61K36/537Salvia (sage)
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K45/00Medicinal preparations containing active ingredients not provided for in groups A61K31/00 - A61K41/00
    • A61K45/06Mixtures of active ingredients without chemical characterisation, e.g. antiphlogistics and cardiaca
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/14Particulate form, e.g. powders, Processes for size reducing of pure drugs or the resulting products, Pure drug nanoparticles
    • A61K9/16Agglomerates; Granulates; Microbeadlets ; Microspheres; Pellets; Solid products obtained by spray drying, spray freeze drying, spray congealing,(multiple) emulsion solvent evaporation or extraction
    • A61K9/1605Excipients; Inactive ingredients
    • A61K9/1629Organic macromolecular compounds
    • A61K9/1641Organic macromolecular compounds obtained otherwise than by reactions only involving carbon-to-carbon unsaturated bonds, e.g. polyethylene glycol, poloxamers
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/14Particulate form, e.g. powders, Processes for size reducing of pure drugs or the resulting products, Pure drug nanoparticles
    • A61K9/16Agglomerates; Granulates; Microbeadlets ; Microspheres; Pellets; Solid products obtained by spray drying, spray freeze drying, spray congealing,(multiple) emulsion solvent evaporation or extraction
    • A61K9/1682Processes
    • A61K9/1694Processes resulting in granules or microspheres of the matrix type containing more than 5% of excipient
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/20Pills, tablets, discs, rods
    • A61K9/2004Excipients; Inactive ingredients
    • A61K9/2022Organic macromolecular compounds
    • A61K9/2027Organic macromolecular compounds obtained by reactions only involving carbon-to-carbon unsaturated bonds, e.g. polyvinyl pyrrolidone, poly(meth)acrylates
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/20Pills, tablets, discs, rods
    • A61K9/2004Excipients; Inactive ingredients
    • A61K9/2022Organic macromolecular compounds
    • A61K9/2031Organic macromolecular compounds obtained otherwise than by reactions only involving carbon-to-carbon unsaturated bonds, e.g. polyethylene glycol, polyethylene oxide, poloxamers
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/20Pills, tablets, discs, rods
    • A61K9/2004Excipients; Inactive ingredients
    • A61K9/2022Organic macromolecular compounds
    • A61K9/205Polysaccharides, e.g. alginate, gums; Cyclodextrin
    • A61K9/2054Cellulose; Cellulose derivatives, e.g. hydroxypropyl methylcellulose
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/20Pills, tablets, discs, rods
    • A61K9/2004Excipients; Inactive ingredients
    • A61K9/2022Organic macromolecular compounds
    • A61K9/205Polysaccharides, e.g. alginate, gums; Cyclodextrin
    • A61K9/2059Starch, including chemically or physically modified derivatives; Amylose; Amylopectin; Dextrin
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/20Pills, tablets, discs, rods
    • A61K9/2095Tabletting processes; Dosage units made by direct compression of powders or specially processed granules, by eliminating solvents, by melt-extrusion, by injection molding, by 3D printing
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/20Pills, tablets, discs, rods
    • A61K9/28Dragees; Coated pills or tablets, e.g. with film or compression coating
    • A61K9/2806Coating materials
    • A61K9/2833Organic macromolecular compounds
    • A61K9/284Organic macromolecular compounds obtained by reactions only involving carbon-to-carbon unsaturated bonds, e.g. polyvinyl pyrrolidone
    • A61K9/2846Poly(meth)acrylates
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/20Pills, tablets, discs, rods
    • A61K9/28Dragees; Coated pills or tablets, e.g. with film or compression coating
    • A61K9/2806Coating materials
    • A61K9/2833Organic macromolecular compounds
    • A61K9/286Polysaccharides, e.g. gums; Cyclodextrin
    • A61K9/2866Cellulose; Cellulose derivatives, e.g. hydroxypropyl methylcellulose
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/20Pills, tablets, discs, rods
    • A61K9/28Dragees; Coated pills or tablets, e.g. with film or compression coating
    • A61K9/2806Coating materials
    • A61K9/288Compounds of unknown constitution, e.g. material from plants or animals
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/48Preparations in capsules, e.g. of gelatin, of chocolate
    • A61K9/50Microcapsules having a gas, liquid or semi-solid filling; Solid microparticles or pellets surrounded by a distinct coating layer, e.g. coated microspheres, coated drug crystals
    • A61K9/5005Wall or coating material
    • A61K9/5015Organic compounds, e.g. fats, sugars
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/48Preparations in capsules, e.g. of gelatin, of chocolate
    • A61K9/50Microcapsules having a gas, liquid or semi-solid filling; Solid microparticles or pellets surrounded by a distinct coating layer, e.g. coated microspheres, coated drug crystals
    • A61K9/5005Wall or coating material
    • A61K9/5021Organic macromolecular compounds
    • A61K9/5026Organic macromolecular compounds obtained by reactions only involving carbon-to-carbon unsaturated bonds, e.g. polyvinyl pyrrolidone, poly(meth)acrylates
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/48Preparations in capsules, e.g. of gelatin, of chocolate
    • A61K9/50Microcapsules having a gas, liquid or semi-solid filling; Solid microparticles or pellets surrounded by a distinct coating layer, e.g. coated microspheres, coated drug crystals
    • A61K9/5005Wall or coating material
    • A61K9/5021Organic macromolecular compounds
    • A61K9/5036Polysaccharides, e.g. gums, alginate; Cyclodextrin
    • A61K9/5042Cellulose; Cellulose derivatives, e.g. phthalate or acetate succinate esters of hydroxypropyl methylcellulose
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/48Preparations in capsules, e.g. of gelatin, of chocolate
    • A61K9/50Microcapsules having a gas, liquid or semi-solid filling; Solid microparticles or pellets surrounded by a distinct coating layer, e.g. coated microspheres, coated drug crystals
    • A61K9/5005Wall or coating material
    • A61K9/5021Organic macromolecular compounds
    • A61K9/5036Polysaccharides, e.g. gums, alginate; Cyclodextrin
    • A61K9/5042Cellulose; Cellulose derivatives, e.g. phthalate or acetate succinate esters of hydroxypropyl methylcellulose
    • A61K9/5047Cellulose ethers containing no ester groups, e.g. hydroxypropyl methylcellulose
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/48Preparations in capsules, e.g. of gelatin, of chocolate
    • A61K9/50Microcapsules having a gas, liquid or semi-solid filling; Solid microparticles or pellets surrounded by a distinct coating layer, e.g. coated microspheres, coated drug crystals
    • A61K9/5005Wall or coating material
    • A61K9/5063Compounds of unknown constitution, e.g. material from plants or animals
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/48Preparations in capsules, e.g. of gelatin, of chocolate
    • A61K9/50Microcapsules having a gas, liquid or semi-solid filling; Solid microparticles or pellets surrounded by a distinct coating layer, e.g. coated microspheres, coated drug crystals
    • A61K9/5089Processes
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P7/00Drugs for disorders of the blood or the extracellular fluid
    • A61P7/02Antithrombotic agents; Anticoagulants; Platelet aggregation inhibitors
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P9/00Drugs for disorders of the cardiovascular system
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P9/00Drugs for disorders of the cardiovascular system
    • A61P9/10Drugs for disorders of the cardiovascular system for treating ischaemic or atherosclerotic diseases, e.g. antianginal drugs, coronary vasodilators, drugs for myocardial infarction, retinopathy, cerebrovascula insufficiency, renal arteriosclerosis

Definitions

  • the present invention relates to a formulation of a micro drop pill and the preparation method thereof, more particularly, the present invention relates to a micro drop pill preparation method with high drug-loading capacity, simple preparation process and high production rate and a formulation of micro drop pill prepared by the method.
  • the method can be used to prepare an uncoated micro drop pill, a coated micro drop pill and a micro drop pill capsule with high drug-loading capacities.
  • Drop pill as an important traditional Chinese medicine preparation, has been used widely. In practice, it has the following merits: shortened production cycle, dust pollution-free, high bioavailability, rapid onset of effect, prolonged action in topical administration, reduced volatility of drug, increased drug stability and being easily carried and stored.
  • the preparation method of the traditional drop pill is to drop a molten medicine liquid into an immiscible cooling medium (in most cases, a coolant is used as the cooling medium) to give the drop pill.
  • a coolant is used as the cooling medium.
  • the unit drug-loading capacity is small (usually, the drug-loading capacity of the active pharmaceutical ingredient (API) is only about 25 wt %) and the amount of matrix used is very large. This cannot meet the requirement of international market that the maximum daily dosage of polyethylene glycols (PEGs) matrix should not exceed 700 mg.
  • the objective of the present invention is to provide a simple and high-speed preparation method to prepare a micro drop pill with high drug-loading capacity and small amount of matrix.
  • the preparation method for preparing the micro drop pill comprises the following steps:
  • Material melting step heat melting a medicine and a drop pill matrix to obtain a molten medicine liquid
  • Another objective of the present invention is to provide a TCM formulation of micro drop pill.
  • the ratio of the medicine to the drop pill matrix is 1:5 ⁇ 5:1 by weight, and the particle size of the micro drop pill is 0.2 mm ⁇ 4 mm.
  • the micro drop pill is prepared according to the preparation method of the micro drop pill of the present invention, and there is no residual coolant.
  • the micro drop pill means that the micro drop pill has a smaller particle size compared with the traditional drop pill. More specifically, the micro drop pill refers to the one with a particle size of 0.2 mm ⁇ 4 mm, especially, the one with a particle size of 0.2 mm ⁇ 2 mm, preferably 1 mm ⁇ 2 mm.
  • the coolant of the drop pill means the coolant commonly-used in the preparation of the traditional drop pill, for example, but not limited to, liquid paraffin, methyl silicone oil and plant oil (soybean oil and castor oil etc.).
  • the medicine includes any one of TCMs or chemicals that is suitable to be prepared into the drop pills.
  • the extract is preferred to be used, e.g. Ginkgo Biloba extract, Bupleurum extract, Salvia Militiorrhiza extract and Andrographis Paniculata extract, as well as the extracts of Qishenyiqi, Huoxiangzhengqi and Compound Salvia Militiorrhiza .
  • These extracts can either be commercially available, or prepared by the method known in the prior art.
  • the micro drop pill includes, but is not limited to: Compound Salvia Militiorrhiza micro drop pill (CSMDP), Qishenyiqi micro drop pill (QMDP), Salvia Militiorrhiza micro drop pill (SMDP), Huoxiangzhengqi micro drop pill (HMDP), Andrographis Paniculata micro drop pill (AMDP), Compound Ginkgo Biloba micro drop pill (CGMDP), Guanxindanshen micro drop pill (GMDP) and Xuesaitong micro drop pill (XMDP) etc.
  • the medicines in the present invention are the API of Compound Salvia Militiorrhiza and the API of Qishenyiqi.
  • Another objective of the present invention is to provide Compound Salvia Militiorrhiza micro drop pill prepared by the method of the present invention, characterized in that the ratio of the API of Compound Salvia Militiorrhiza to the drop pill matrix is 1:5 ⁇ 5:1 by weight, and a particle size of the micro drop pill is 0.2 mm ⁇ 4 mm, preferably 0.2 mm ⁇ 2 mm, more preferably 1 mm ⁇ 2 mm.
  • the API of Compound Salvia Militiorrhiza is prepared with the following crude drugs by weight parts: Salvia Militiorrhiza 75.0 ⁇ 90.0 parts, Panax Notoginseng 10.0 ⁇ 25.0 parts and borneol 0.1 ⁇ 4.0 parts, and is prepared by the preparation method for the micro drop pill of the present invention. There is no residual coolant in the micro drop pills.
  • the API of Qishenyiqi is prepared by the following crude drugs by weight parts: Astragalus membranaceus 100 ⁇ 200 parts, Salvia Militiorrhiza 50 ⁇ 100 parts, Panax Notoginseng 10 ⁇ 20 parts and volatile oil from Lignum Dalbergiae Odoriferae 0.5 ⁇ 2 parts, and is prepared by the preparation method for the micro drop pill of the present invention. There is no residual coolant in the micro drop pills.
  • the present invention is achieved by the following technical solutions:
  • a preparation method for a micro drop pill comprising the following steps:
  • Material melting step heat melting a medicine and a drop pill matrix to obtain a molten medicine liquid
  • Material melting step heat melting the medicine and the drop pill matrix at 40° C. ⁇ 120° C., homogenizing for 0.5 ⁇ 4 hours to obtain a homogenized molten medicine liquid, and the ratio of the medicine to the drop pill matrix is 1:5 ⁇ 5:1 by weight;
  • Condensation step cooling the medicine drops with a cooling gas for forming by solidifying, obtaining micro drop pills having a particle size of 0.2 mm ⁇ 4 mm, the temperature of the cooling gas is 0° C. or lower.
  • the drop pill matrix includes one or more selected from the group consisting of PEGs, sorbitol, xylitol, lactitol, maltose, starch, methylcellulose, sodium carboxymethyl cellulose, hydroxypropyl methylcellulose (HPMC), arabic gum, alginic acid, dextrin, cyclodextrin, agar and lactose; preferably solid PEGs, such as PEG-1000, PEG-2000, PEG-3000, PEG-4000, PEG-5000, PEG-6000, PEG-7000 and PEG-8000; more preferably one or more selected from the group consisting of PEG-1000, PEG-2000, PEG-3000, PEG-4000, PEG-6000 and PEG-8000; most preferably PEG-6000, PEG-4000 or the combination of PEG-4000 and PEG-6000.
  • PEGs sorbitol, xylitol, lactitol, maltose, starch, methylcellulose
  • Step (1) the temperature for heat melting is at 60 ⁇ 100° C., more preferably at 65 ⁇ 90° C., further preferably 75 ⁇ 85° C.
  • the homogenizing time preferably is 1 ⁇ 3 hours, further preferably 2 hours.
  • Step (1) the ratio of the medicine to the drop pill matrix is 1:3 ⁇ 3:1 by weight, preferably 1:(1 ⁇ 3) by weight.
  • Step (2) the temperature of the dripper is at 40 ⁇ 120° C., preferably at 40 ⁇ 100° C.; the vibration frequency for dropping is preferably at 20 ⁇ 300 Hz, more preferably 50 ⁇ 300 Hz, more preferably 20 ⁇ 200 Hz, more preferably 20 ⁇ 150 Hz, most preferably 50 ⁇ 150 Hz; the vibration mode includes magnetic/electronic vibration or pneumatic vibration.
  • Step (3) the temperature of the cooling gas is at 0° C. ⁇ 150° C., preferably ⁇ 10 ⁇ 140° C., further preferably ⁇ 40° C. ⁇ 140° C., further preferably ⁇ 60° C. ⁇ 140° C., most preferably ⁇ 80° C. ⁇ 120° C.; and the cooling gas is air, nitrogen or inert gas.
  • Step (3) the particle size of the micro drop pill is 1.0 mm ⁇ 2.0 mm, preferably 0.5 mm ⁇ 2 mm.
  • Material melting step heat melting the medicine and the drop pill matrix at 60° C. ⁇ 100° C., homogenizing for 1 ⁇ 3 hours to obtain a homogenized molten medicine liquid, the ratio of the medicine to the drop pill matrix is 1:3 ⁇ 3:1 by weight;
  • Material melting step charging the medicine and the drop pill matrix into a homogenizer, mixing homogenously at 1000 ⁇ 5000 rpm for 1 ⁇ 200 min, then melting homogenously at 3000 ⁇ 10000 rpm for 1 ⁇ 100 min; during the melting process, the temperature is kept at 60 ⁇ 100° C. to obtain the molten medicine liquid; the ratio of the medicine to the drop pill matrix is 1:5 ⁇ 5:1 by weight;
  • Step (2) Dropping step: delivering the molten medicine liquid under pressure to the dripper, and acquiring medicine drops from the dripper by means of vibration dropping at a vibration frequency of 20 ⁇ 300 Hz under a dropping pressure of 0.5 ⁇ 4.0 Bar and the temperature of the dripper of 40° C. ⁇ 200° C., the dropping rate is matched with the melting rate in Step (1);
  • Step (1) the ratio of the medicine to the drop pill matrix is 1:3 ⁇ 3:1 by weight, mixing homogeneously at 3000 ⁇ 5000 rpm for 10 ⁇ 60 min, then melting homogeneously at 4000 ⁇ 9000 rpm for 5 ⁇ 30 min, during the melting process, the temperature is kept at 70 ⁇ 90° C.
  • Step (1) the ratio of the medicine to the drop pill matrix is 1:(1 ⁇ 3) by weight, mixing homogeneously at 3000 ⁇ 4000 rpm for 10 ⁇ 30 min, then melting homogeneously at 4000 ⁇ 6000 rpm for 6 ⁇ 30 min, during the melting process, the temperature is kept at 75 ⁇ 85° C.
  • Step (2) the temperature of the dripper is at 70 ⁇ 100° C.
  • the vibration frequency for dropping is at 90 ⁇ 200 Hz
  • the dropping pressure is at 1.0 ⁇ 3.0 Bar; preferably the vibration frequency is at 137 Hz, an acceleration speed is at 4G, the dropping pressure is at 1.8 Bar and the temperature of the dripper is at 75 ⁇ 85° C.
  • the dropping rate is 10 ⁇ 40 Kg/h, preferably 12 ⁇ 30 Kg/h, further preferably 15 ⁇ 25 Kg/h.
  • Step (4) drying the low-temperature drop pills from Step (3) on a fluidized-bed at 40 ⁇ 150° C., preferably at 40 ⁇ 60° C. for 1 ⁇ 4 hours, preferably 1 ⁇ 3 hours, most preferably 2 hours to obtain uncoated drop pills.
  • Step (4) a gradient-rising temperature drying method is used as follows: fluidizing at ⁇ 20 ⁇ 30° C., drying at 15 ⁇ 35° C. for 10 ⁇ 120 min, drying at 35 ⁇ 55° C. for 10 ⁇ 60 min, drying at 55 ⁇ 100° C. for 0 ⁇ 60 min; preferably, the gradient-rising temperature drying method is performed as follows: fluidizing at 0 ⁇ 20° C., drying at 25° C. for 60 min, drying at 45° C. for 30 min, drying at 55° C. for 0 ⁇ 30 min.
  • the method additionally comprises a coating step as Step (5): coating the uncoated drop pills obtained from Step (4) in a state of fluidization; the concentration of the coating liquid is at 15 ⁇ 25 wt %, preferably 18 ⁇ 20 wt %; the coating material is selected from shellac, CAP (cellulose acetate phthalate), methyl acrylate, methyl methacrylate or Opadry; the ratio of the coating material to the uncoated drop pill is 1:50 ⁇ 1:25 by weight.
  • a coating step as Step (5) coating the uncoated drop pills obtained from Step (4) in a state of fluidization; the concentration of the coating liquid is at 15 ⁇ 25 wt %, preferably 18 ⁇ 20 wt %; the coating material is selected from shellac, CAP (cellulose acetate phthalate), methyl acrylate, methyl methacrylate or Opadry; the ratio of the coating material to the uncoated drop pill is 1:50 ⁇ 1:25 by weight.
  • Step (1) adding the medicine powder or extract with water, stirring for 10 min or longer at 30 ⁇ 80° C. to obtain a pre-mixed medicine material.
  • the present invention includes the following technical solutions:
  • a TCM formulation of micro drop pill wherein in the micro drop pill, the ratio of the medicine to the drop pill matrix is 1:5 ⁇ 5:1 by weight, a particle size of the micro drop pill is 0.2 mm ⁇ 4 mm, the micro drop pill is prepared by any one method of the 1 st ⁇ 19 th paragraphs, and the micro drop pill has no residual coolant.
  • TCM formulation of micro drop pill according to the 20 th paragraph characterized in that the particle size is 0.2 mm ⁇ 2 mm.
  • TCM formulation of micro drop pill according to the 21 st paragraph characterized in that the particle size is 1 mm ⁇ 2 mm.
  • a Compound Salvia Militiorrhiza micro drop pill wherein the micro drop pill is prepared by the API of Compound Salvia Militiorrhiza and the drop pill matrix in a ratio of 1:5 ⁇ 5:1 by weight, the particle size of the Compound Salvia Militiorrhiza micro drop pill is 0.2 mm ⁇ 4 mm, the API of Compound Salvia Militiorrhiza is prepared by the following crude drugs by weight parts: Salvia Militiorrhiza 75.0 ⁇ 90.0 parts, Panax Notoginseng 10.0 ⁇ 25.0 parts and borneol 0.1 ⁇ 4.0 parts, and the micro drop pill is prepared by any one method of the 1 st ⁇ 19 th paragraphs, and the micro drop pill has no residual coolant.
  • CSMDP Compound Salvia Militiorrhiza micro drop pill
  • micro drop pill is prepared by the API of Compound Salvia Militiorrhiza and the drop pill matrix in a ratio of 1:3 ⁇ 3:1 by weight.
  • micro drop pill is prepared by the API of Compound Salvia Militiorrhiza and the drop pill matrix in a ratio of 1:(1 ⁇ 3) by weight.
  • a Qishenyiqi micro drop pill characterized in that the micro drop pill is prepared by the API of Qishenyiqi and the drop pill matrix in a ratio of 1:5 ⁇ 5:1 by weight, the particle size of the Qishenyiqi micro drop pill is 0.2 mm ⁇ 4 mm, the API is prepared by the following crude drugs by weight parts: Astragalus membranaceus 100 ⁇ 200 parts, Salvia Militiorrhiza 50 ⁇ 100 parts, Panax Notoginseng 10 ⁇ 20 parts and volatile oil from Lignum Dalbergiae Odoriferae 0.5 ⁇ 2 parts, the micro drop pill is prepared by any one method of the 1 st ⁇ 19 th paragraphs, and the micro drop pill has no residual coolant.
  • QMDP Qishenyiqi micro drop pill
  • the preparation method for preparing the micro drop pill comprises the following steps:
  • Material melting step heat melting the medicine and the drop pill matrix at 40° C. ⁇ 120° C., homogenizing for 0.5 ⁇ 4 hours to obtain a homogenized molten medicine liquid, the ratio of the medicine to the drop pill matrix is 1:5 ⁇ 5:1 by weight;
  • the drop pill matrix includes one or more selected from the group consisting of PEGs, sorbitol, xylitol, lactitol, maltose, starch, methylcellulose, sodium carboxymethyl cellulose, hydroxypropyl methylcellulose (HPMC), arabic gum, alginic acid, dextrin, cyclodextrin, agar and lactose, preferably solid PEGs, such as PEG-1000, PEG-2000, PEG-3000, PEG-4000, PEG-5000, PEG-6000, PEG-7000 and PEG-8000, more preferably one or more selected from the group consisting of PEG-1000, PEG-2000, PEG-3000, PEG-4000, PEG-6000, PEG-8000, most preferably PEG-6000, PEG-4000 or the combination of PEG-4000 and PEG-6000.
  • PEGs sorbitol, xylitol, lactitol, maltose, starch, methylcellulose
  • the temperature for heat melting preferably is at 60 ⁇ 100° C., more preferably at 65 ⁇ 90° C., further preferably 75 ⁇ 85° C.
  • the homogenizing time preferably is 1 ⁇ 3 hours, further preferably 2 hours.
  • the ratio of the medicine to the drop pill matrix is 1:3 ⁇ 3:1 by weight, preferably 1:(1 ⁇ 3) by weight.
  • the temperature of the dripper is preferably at 60 ⁇ 120° C., preferably at 60 ⁇ 100° C.; the vibration frequency for dropping is preferably at 20 ⁇ 300 Hz, more preferably 50 ⁇ 300 Hz, more preferably 20 ⁇ 200 Hz, more preferably 20 ⁇ 150 Hz, most preferably 50 ⁇ 150 Hz.
  • the vibration mode includes magnetic/electronic vibration or pneumatic vibration. Wherein, in the pneumatic vibration mode, the vibration frequency and the vibration amplitude are larger. If the material viscosity is more than 800 cp, the electronic vibration is incapable of effectively cutting material, resulting in the blockage of the dripper; if this happens, the pneumatic vibration mode can be used.
  • the electronic vibration is preferably employed, the viscosity of the molten medicine liquid preferably is 500 ⁇ 1000 cp, more preferably 700 ⁇ 1000 cp.
  • a vibration waveform is used as a PAT (Process Analyzing Technology) index to measure the distribution of the particle size and to monitor the state of fluidization of the drop pills in the real-time manner by using a stroboscopic device.
  • PAT Process Analyzing Technology
  • the condensation by a cooling gas means that the drops are cooled by using a low-temperature condensate trap to form by solidifying.
  • the temperature of the cooling gas is at 0° C. ⁇ 150° C., preferably ⁇ 10° C. ⁇ 140° C., further preferably ⁇ 40° C. ⁇ 140° C., further preferably ⁇ 60° C. ⁇ 140° C., most preferably ⁇ 80° C. ⁇ 120° C.;
  • the cooling gas is air, nitrogen or inert gas;
  • the particle size of the micro drop pill is 1.0 mm ⁇ 2.0 mm, preferably 0.5 mm ⁇ 2 mm.
  • the preparation method for preparing the micro drop pill comprises the following steps:
  • Material melting step heat melting the medicine and the drop pill matrix at 60° C. ⁇ 100° C., homogenizing for 1 ⁇ 3 hours to obtain a homogenized molten medicine liquid, the ratio of the medicine to the drop pill matrix is 1:3 ⁇ 3:1 by weight;
  • the preparation method for preparing the micro drop pill comprises the following steps:
  • Material melting step charging the medicine and the drop pill matrix into a homogenizer, mixing homogenously at 1000 ⁇ 5000 rpm for 1 ⁇ 200 min, then melting homogenously at 3000 ⁇ 10000 rpm for 1 ⁇ 100 min; during the melting process, the temperature is kept at 60 ⁇ 100° C. to obtain the molten medicine liquid; the ratio of the medicine to the drop pill matrix is 1:5 ⁇ 5:1 by weight;
  • Step (2) Dropping step: delivering the molten medicine liquid to a dripper, and acquiring medicine drops by means of vibration dropping at a vibration frequency for dropping of 20 ⁇ 300 Hz under a dropping pressure of 0.5 ⁇ 4.0 Bar and the temperature of the dripper of 40° C. ⁇ 200° C.; the dropping rate is matched with the melting rate in Step (1); and,
  • the ratio of the medicine to the drop pill matrix is 1:3 ⁇ 3:1 by weight, mixing homogeneously 3000 ⁇ 5000 rpm for 10 ⁇ 60 min and melting homogeneously at 4000 ⁇ 9000 rpm for 5 ⁇ 30 min, during the melting process, the temperature is kept at 70 ⁇ 90° C.; most preferably, the ratio of the medicine to the drop pill matrix is 1:(1 ⁇ 3) by weight, mixing homogeneously 3000 ⁇ 4000 rpm for 10 ⁇ 30 min and melting homogeneously at 4000 ⁇ 6000 rpm for 6 ⁇ 30 min, during the melting process, the temperature is kept at 75 ⁇ 85° C.
  • the temperature of the dripper is at 70 ⁇ 100° C.
  • the vibration frequency for dropping is at 90 ⁇ 200 Hz
  • the dropping pressure is at 1.0 ⁇ 3.0 Bar
  • the vibration frequency is at 137 Hz
  • the acceleration speed is at 4G
  • the dropping pressure is at 1.8 Bar
  • temperature of the dripper is at 75 ⁇ 85° C.
  • the dropping rate is 10 ⁇ 40 Kg/h, preferably 12 ⁇ 30 Kg/h, further preferably 15 ⁇ 25 Kg/h.
  • the method can additionally comprise a drying step as Step (4): drying the low-temperature drop pills from Step (3) on a fluidized-bed at 40 ⁇ 150° C., preferably at 40 ⁇ 60° C. for 1 ⁇ 4 hours, preferably 1 ⁇ 3 hours, most preferably 2 hours to obtain the uncoated drop pills.
  • a gradient-rising temperature drying method is used as follows: fluidizing at ⁇ 20 ⁇ 30° C., drying at 15 ⁇ 35° C. for 10 ⁇ 120 min, drying at 35 ⁇ 55° C. for 10 ⁇ 60 min, drying at 55 ⁇ 100° C. for 0 ⁇ 60 min; preferably, the gradient-rising temperature drying method is performed as follows: fluidizing at 0 ⁇ 20° C., drying at 25° C. for 60 min, drying at 45° C. for 30 min, drying at 55° C. for 0 ⁇ 30 min.
  • Step (4) by screening from a large number of drying methods, the inventors found that: in Step (3), the uncoated drop pill is dried by one of the following drying methods: airing under low-humidity, drying by coating pot, drying by vacuum drying oven, drying by hot air circulation drying oven, drying by track type microwave dryer, drying by fluidized drying coater.
  • airing under low-humidity drying by coating pot, drying by vacuum drying oven, drying by hot air circulation drying oven, drying by track type microwave dryer, drying by fluidized drying coater.
  • drying by coating pot, drying by track type microwave dryer, drying by fluidized drying coater are preferred.
  • drying by fluidized-bed is preferred, and drying by fluidized drying coater is more preferred. Advantages and disadvantages of various drying methods are shown in Table 1.
  • the yield is usually (1) Stringent requirement for airing environment, low-humidity about 95% without considering the demanding clean air-circulated workshops with a effect of dropping factor. relative humidity of less than 30%, a temperature of higher than 20° C. and a good air circulation; (2) Prolonged drying period, at least 48 hours required when a layer thickness of the drop pills is up to about 2 cm; (3) Large-area workshop is occupied; (4) Regularly turning the drop pills is necessary; (5) Exposing for a long time, the drop pill product is prone to being polluted. 2 Drying by (1) High yield.
  • the yield is usually (1) Demanding the inlet air having a low humidity, coating pot about 95% without considering the generally no more than 5 g/kg; effect of dropping factor; (2) Low drying efficiency, at least 6 h/batch; (2) Drying and coating can be achieved (3) Custom-made device; in one machine. (4) Easily resulting in product rejection due to the adhesion of drop pills. 3 Drying by vacuum None (1) Low drying efficiency, demanding low-temperature drying oven vacuum drying for a long time, at least 30 h/batch; (2) Low-productivity device, the productivity of oven per square meter is difficult to exceed 0.2 kg/h; (3) hardly resulting in adhesion and deformation of drop pills, which is not round in appearance.
  • the preparation method for the micro drop pill can additionally comprise a coating step as Step (5): coating the uncoated drop pills obtained from Step (4) in a state of fluidization; the concentration of the coating liquid is at 15 ⁇ 25 wt %, preferably 18 ⁇ 20 wt %; the coating material is selected from shellac, CAP (cellulose acetate phthalate), methyl acrylate, methyl methacrylate or Opadry; the ratio of the coating material to the uncoated drop pills is 1:50 ⁇ 1:25 by weight.
  • a coating step (5) coating the uncoated drop pills obtained from Step (4) in a state of fluidization; the concentration of the coating liquid is at 15 ⁇ 25 wt %, preferably 18 ⁇ 20 wt %; the coating material is selected from shellac, CAP (cellulose acetate phthalate), methyl acrylate, methyl methacrylate or Opadry; the ratio of the coating material to the uncoated drop pills is 1:50 ⁇ 1:25 by weight
  • the method in order to better implement the preparation method for the micro drop pill, preferably, can additionally comprise a pre-mixing step before Step (1): adding the medicine powder or extract with water, stirring for 10 min or longer at 30 ⁇ 80° C. to obtain a pre-mixed medicine material, ensuring the homogenization of water content.
  • This step can remedy the defects brought about by feeding dried powder material.
  • the micro drop pills prepared by the method can be either packaged directly, or prepared into capsule after loading into a capsule shell.
  • the weighing step for capsules one-by-one may be additionally employed. Before packaging, high-speed weighing for the loaded capsules one-by-one is employed so as to eliminate possibly unqualified capsules.
  • the features of the method are as follows: it is the first time to combine the techniques of vibration dropping and gas cooling with the fluidized drying & coating method creatively and apply to the preparations of drop pills and drop pill capsules. Hence, both producing rate and forming quality of the drop pill are increased.
  • Utilization of gas cooling well meets the requirements of high-speed dropping, preparing a micro drop pill (with a particle size of 2.5 mm or smaller) and increasing drug-loading capacity.
  • the drug-loading capacity of the drop pill has been increased by folds while the amount of the drop pill matrix and the dosage are reduced dramatically.
  • the productivity of the drop pills has been enhanced greatly from the traditional rate of 1 ⁇ 2 pills/s to 1000 ⁇ 1250 pills/s, and the range of the particle size is expanded from 2 mm ⁇ 4 mm to 0.2 mm ⁇ 4 mm. It is possible to produce the micro drop pills that can better meet the requirements for capsule loading.
  • the vibration parameters and fluidized drug loading coating the drug-loading capacity can be increased from about 25 wt % of the traditional drop pills to 50 wt % and higher, and the amount of the drop pill matrix is also reduced by leaps and bounds.
  • fluidized drying & coating process not only can solve the problems during the storage of the drop pills prepared by air drying method such as possible adhesion of the drop pills from each other, precipitation of components and reduced volatile oil components, but also the drying time can be reduced from 4 ⁇ 24 hours to only 2 hours.
  • the molten medicine liquid was injected to make drug-loading coating, and the drug-loading capacity can be further increased.
  • this technique of injection can be used for coating the drop pills so as to realize the purposes of different techniques (e.g. sustained release coating, film coating and sugar coating etc). Because the fluidization is a mild process, it ensures the water content in the drop pill reaches a stable value, and the uniformity in drug-loading and coating in the drop pills are also improved. Unlike the drop pills prepared by the traditional methods, the fluidization can prevent the drop pills from being cleft and white-dotted, and at the same time, the yield is increased.
  • Compound Salvia Militiorrhiza Drop Pill is a TCM developed by Tianjin Tasly Pharmaceutical Co., Ltd, which is proven to have effects of activating blood by removing stasis and stopping pain by regulating Qi, used for treating chest distress and angina pectoris.
  • the main ingredients of Compound Salvia Militiorrhiza Drop Pill include Salvia Militiorrhiza, Panax Notoginseng and borneol. Its pharmacological effects include increasing coronary blood flow, protecting ischemia myocardium by strengthening hypoxia tolerance, preventing thrombosis by anti-platelet aggregation and improving microcirculation etc.
  • the current Compound Salvia Militiorrhiza Drop Pill was prepared by the following method: extracting Salvia Militiorrhiza and Panax Notoginseng with water to give an extraction liquid, which was followed by concentration to get the extract; mixing the extract with the drop pill matrix, delivering to a dropping machine, into which borneol was added and well mixed to get a material; melting and dropping the material, and cooling the medicine drops by using liquid paraffin as a coolant to obtain Compound Salvia Militiorrhiza Drop Pill.
  • the preparation of Compound Salvia Militiorrhiza Drop Pill was known as a very mature technique by the person skilled in the art, there were still a lot of problems faced during the preparation process, e.g. large amount of the matrix and a small unit drug-loading capacity.
  • the CSMDP is prepared by the API of Compound Salvia Militiorrhiza and the drop pill matrix in a ratio of 1:5 ⁇ 5:1 by weight; preferably 1:3 ⁇ 3:1 by weight; most preferably 1:(1 ⁇ 3) by weight.
  • the API of Compound Salvia Militiorrhiza is prepared by the following crude drugs by weight parts:
  • the API of Compound Salvia Militiorrhiza is prepared by the following crude drugs by weight parts:
  • Panax Notoginseng 15.0 ⁇ 18.0 parts borneol 0.2 ⁇ 2.0 parts.
  • the API of Compound Salvia Militiorrhiza is prepared by the following crude drugs by weight parts:
  • the API of Compound Salvia Militiorrhiza is believed to be the active pharmaceutical ingredient of CSDP, which is prepared by extracting Salvia Militiorrhiza and Panax Notoginseng to give the extract and mixing borneol to obtain the product.
  • the preparation of the API belongs to the prior art, and the API can be prepared by the conventional methods with the crude drugs in the ratios of the present invention, or by the commercially available Salvia Militiorrhiza extract, Panax Notoginseng extract and borneol.
  • the API of Compound Salvia Militiorrhiza is preferably prepared by the following method:
  • Step (1) under an alkaline condition, Salvia Militiorrhiza and Panax Notoginseng are decocted for 1 ⁇ 3 times, 1 ⁇ 3 hours each time and the decoction is filtered to get a filtrate (Filtrate I) for later use; dregs of the decoction is further decocted with water for 1 ⁇ 3 times, 1 ⁇ 3 hours each time, the decoction is filtered to get a filtrate (Filtrate II) for later use; Filtrate I and Filtrate II are combined and concentrated to give a concentrated liquid, which is precipitated with ethanol and allows to stand still to get a supernatant; the supernatant is filtered, ethanol therein is recovered, and further concentrated to give the Salvia Militiorrhiza and Panax Notoginseng extract.
  • the alkaline condition includes, but not limited to, one or more kinds alkali selected from the group consisting of sodium bicarbonate, sodium carbonate, disodium hydrogen phosphate, sodium dihydrogen phosphate, sodium hydroxide, potassium hydroxide and magnesium hydroxide; a pH value of 7.5 ⁇ 9.0 is preferred, ensuring sodium danshensu (sodium DL-beta-(3,4-dihydroxyphenyelactate) can be extracted totally.
  • ⁇ 100% (v/v) (most preferably 95% (v/v)) ethanol solution is added to perform ethanol-precipitation, the final content of ethanol preferably is 60 ⁇ 75% (v/v).
  • the preparation method for preparing the CSMDP comprises the following steps:
  • Material melting step charging the API of Compound Salvia Militiorrhiza and the drop pill matrix in a ratio of 1:5 ⁇ 5:1 by weight into a homogenizer, mixing homogenously at 1000 ⁇ 5000 rpm for 1 ⁇ 200 min, then melting homogenously at 3000 ⁇ 10000 rpm for 1 ⁇ 100 min; during the melting process, the temperature is kept at 60 ⁇ 100° C. to obtain a molten medicine liquid;
  • Step (2) Dropping step: delivering the molten medicine liquid to a dripper, and acquiring medicine drops by means of vibration dropping at a vibration frequency of 50 ⁇ 300 Hz under a dropping pressure of 0.5 ⁇ 4.0 Bar, the temperature of the dripper is at 70° C. ⁇ 200° C.; the dropping rate is matched with the melting rate in Step (1); and,
  • Step (2) and Step (3) the pill weight is decreased from 23.5 ⁇ 27.5 mg of the traditional drop pill to 3 ⁇ 4 mg, which can be loaded into capsules; in addition, the problem of residual coolant such as liquid paraffin in the current drop pill product can be solved by using gas cooling.
  • CSMDP of the present invention was prepared by the method of Preparative Example 1 of CSMDP.
  • CSDP used as a comparative drug, was commercially available in China, prepared by Tianjin Tasly Pharmaceutical Co., Ltd.
  • TTC triphenyl tetrazolium chloride
  • Grouping the rats were randomly divided into groups according to their body weight: S group (Sham operation group), M group (Model group), Y group (Positive control group, metoprolol tartrate, Lot No. 1201039), F group (CSMDP of the present invention) and G group (CSDP available in China, Lot No. 2011L16); 10 rats in each group.
  • the animals were administrated intragastrically for 7 days, which was shown in Table 3.
  • Chest on the left front chest lateral side was incised to cut the 3′ rib and the pericardium was carefully lifted with forceps to tear apart.
  • LAD left anterior decending branch
  • Medical suture (4-0) was used to transfix LAD and a small amount of myocardial tissue at a distance of about 1 ⁇ 2 mm from the lower edge of the left atrial appendage and inside interventricular sulcus in the vicinity of the left main trunk of coronary vein.
  • Chest was closed layer by layer. The tracheal tube was removed until the voluntary respiration was recovered in the rats. ECG was recorded continuously for 4 hours. Rats were anesthetized, their heart were cut out, sliced and dyed to calculate myocardial infarction rate (MIR). The serum was collected for later use.
  • MIR myocardial infarction rate
  • MIR (%) wet weight of the infarction region/wet weight of the whole heart ⁇ 100%
  • the descending order of the heart rate was F group, G group, M group, Y group and S group within the observation period and 0 ⁇ 1 hour after ligation. 1 hour later, the heart rate in each group was decreased. Within the observation period, the variation of heart rate in Y group and S group was relatively stable. There was no significant difference among these groups in heart rate of the rats.
  • the medicines in each group were proven to have a certain effect against myocardial infarction in the rats with a coronary artery ligature; especially the CSMDP of the present invention at a dosage of 84 mg/kg had a MIR of 3.38 ⁇ 0.49%, having a similar efficacy of MIR (3.32 ⁇ 0.59%) of the CSDP product commercially available in China at a dosage of 115 mg/kg.
  • the CSMDP at a dosage of 84 mg/kg reached the same effect with the CSDP product commercially available in China at a dosage of 115 mg/kg.
  • the CSMDP had a better efficacy than the current CSDP, having the merits such as high bioavailability, reduced administration dosage and good compliance to the patients, etc.
  • the following materials were prepared: 75 g of Salvia Militiorrhiza and Panax Notoginseng extract, 7.5 g of borneol and 165 g of PEG-6000.
  • Pre-mixing step the API of Compound Salvia Militiorrhiza was added with water to pre-mix, stirred in a heat-insulated tank at 40 ⁇ 10° C. for 60 min or longer to make the water content of the API of Compound Salvia Militiorrhiza at 13.0 wt % to give a pre-mixed material of the API of Compound Salvia Militiorrhiza for later use;
  • Step (3) Dropping step: the aforesaid molten medicine liquid was delivered to a dripper, the vibration frequency of the dripper was adjusted to 137 Hz and the temperature of the dripper was adjusted to 80° C.; the medicine liquid was flowed under pressure (1.8 Bar) into the dripper, from the bottom of which the medicine liquid was dropped down by means of vibration; the dropping rate was matched with the melting rate in Step (1);
  • Drying step the resultant drop pills were dried in a fluidized state; until the drop pills reached a better fluidized state in the bed of the fluidized bed, the temperature was increased to 25° C. to dry for 60 min, further increased to 45° C. to dry for 30 min, continuously increased to 55° C. to dry for 30 min, and decreased 30° C. or lower to discharge the drop pills.
  • the water content of the drop pills was controlled in the range of 3.0 ⁇ 7.0 wt % to give uncoated drop pills as the intermediate product;
  • Coating step the amount of coating powder was calculated based on the coating feed capacity and formulation; Opadry, which has 4 wt % of the weight of the uncoated drop pills, was used to prepare a 18 wt % coating solution and stirred for 45 min; the inlet air temperature was initially set to 25° C.; after the qualified uncoated drop pills were loaded into the fluidized bed, the inlet air temperature was increased to 48° C.; until the temperature of the materials was up to 38° C., the coating was started; the temperature of the material was kept at 35 ⁇ 45° C. during the coating and decreased 30° C.
  • the drop pills were discharged, screened to give coated drop pills as the intermediate product, the coating weigh of the coated drop pills was controlled in a range of 3.3 ⁇ 0.7 wt % and the water content was controlled in a range of 3.0 ⁇ 7.0 wt %;
  • the formation of the drop pills was measured visually by using a stroboscopic illumination to perform a real-time monitoring and adjustment.
  • the steps of screening and regulating the drop pills could be added.
  • API of Compound Salvia Militiorrhiza was prepared by the following method:
  • Step (1) under an alkaline condition (pH 8.0), Salvia Militiorrhiza and Panax Notoginseng were decocted for 2 times, 2 hours each time and filtered to give Filtrate I for later use; dregs of the decoction was further decocted with water for 2 times, 2 hours each time, filtered to give Filtrate II for later use; Filtrate I and Filtrate II were combined and concentrated to give a concentrated liquid, which was added with ethanol to make the final content of ethanol as 70% (v/v) and allowed to stand still to give a supernatant; the supernatant was taken, filtered, ethanol therein was recovered, concentrated and dried to give the Salvia Militiorrhiza and Panax Notoginseng extract.
  • an alkaline condition pH 8.0
  • the CSMDP was prepared by the same method as CSMDP PREPARATIVE EXAMPLE 1.
  • the CSMDP was prepared by the same method as CSMDP PREPARATIVE EXAMPLE 1.
  • CSMDP was prepared by the following steps:
  • Material melting step the mixture of cyclodextrin and agar (1:1) was used as a matrix, charged into a homogenizer with the API of Compound Salvia Militiorrhiza to homogenize at 1000 rpm for 1 min to give a material; the material was molten homogenously at 3000 rpm for 1 min; during the melting process, the temperature of the material was kept at 60° C. to obtain a molten medicine liquid;
  • Step (2) Dropping step: the molten medicine liquid was delivered to a dripper and dropped by means of vibration dropping at the dripper temperature of 70° C. and a vibration frequency of 50 Hz under a dropping pressure of 0.5 Bar; the dropping rate was matched with the melting rate in Step (1); and,
  • CSMDP was prepared by the following steps:
  • Material melting step the mixture of arabic gum and lactose (1:1) was used as a matrix, charged into a homogenizer with the API of Compound Salvia Militiorrhiza to homogenize at 5000 rpm for 200 min to give a material; the material was molten homogenously at 10000 rpm for 100 min; during the melting process, the temperature of the material was kept at 100° C. to obtain a molten medicine liquid;
  • Step (2) the molten medicine liquid was delivered to a dripper and dropped by means of vibration dropping at the dripper temperature of 300° C. and a vibration frequency of 300 Hz under a dropping pressure of 4.0 Bar; the dropping rate was matched with the melting rate in Step (1); and,
  • CSMDP was prepared by the following steps:
  • Material melting step the lactitol was used as a matrix, charged into a homogenizer with the API of Compound Salvia Militiorrhiza to homogenize at 2500 rpm for 100 min to give a material; the material was molten homogenously at 6000 rpm for 50 min; during the melting process, the temperature of the material was kept at 80° C. to obtain the molten medicine liquid;
  • Step (2) Dropping step: the molten medicine liquid was delivered to a dripper and dropped by means of vibration dropping at the dripper temperature of 150° C. and a vibration frequency of 150 Hz under a dropping pressure of 2 Bar; the dropping rate was matched with the melting rate in Step (1);
  • Coating step the resultant dried uncoated drop pills were coated at 40° C. in fluidized bed to obtain coated drop pills; the ratio of the coating material to the uncoated drop pills was 1:25 by weight; the concentration of the coating solution was 10 wt % and the coating material was Opadry.
  • CSMDP was prepared by the following steps:
  • API powder of Compound Salvia Militiorrhiza was added with water and stirred at 60° C. for 10 min or longer to obtain a pre-mixed API of Compound Salvia Militiorrhiza.
  • Material melting step the PEG-8000 and the pre-mixed API of Compound Salvia Militiorrhiza were charged into a homogenizer to homogenize at 2500 rpm for 100 min to give a material; the material was molten homogenously at 6000 rpm for 50 min; during the melting process, the temperature of the material was kept at 80° C. to obtain a molten medicine liquid;
  • Step (2) the molten medicine liquid was delivered to a dripper and dropped by means of vibration dropping at a dripper temperature of 150° C. and a vibration frequency of 150 Hz under a dropping pressure of 2 Bar; the dropping rate was matched with the melting rate in Step (1);
  • Coating step the resultant dried uncoated drop pills were coated at 40° C. in fluidized bed to obtain coated drop pills; the ratio of the coating material to the dried uncoated drop pills was 1:25 by weight; the concentration of the coating solution was 10 wt % and the coating material was shellac.
  • CSMDP was prepared by the following steps:
  • API powder of Compound Salvia Militiorrhiza was added with water and stirred at 30° C. for 10 min or longer to obtain a pre-mixed API of Compound Salvia Militiorrhiza.
  • Material melting step the PEG-1000 and the pre-mixed API of Compound Salvia Militiorrhiza were charged into a homogenizer to homogenize at 2500 rpm for 100 min to give a material; the material was molten homogenously at 6000 rpm for 20 min; during the melting process, the temperature of the material was kept at 100° C. to obtain a molten medicine liquid;
  • Step (2) the molten medicine liquid was delivered to a dripper and dropped by means of vibration dropping at a dripper temperature of 70° C. and a vibration frequency of 100 Hz under a dropping pressure of 1.0 Bar and an acceleration speed of 1G and a dropping rate of 10 Kg/h; the dropping rate was matched with the melting rate in Step (1);
  • the resultant drop pills were dried by a gradient-rising temperature drying method, fluidized at ⁇ 20° C., dried at 15° C. for 10 min, further dried at 35° C. for 10 min, and further dried at 55° C. for 30 min to give dried uncoated drop pills; and,
  • Coating step the resultant dried uncoated drop pills were coated at 40° C. in a fluidized bed to obtain coated drop pills; the ratio of the coating material to the dried uncoated drop pills was 1:25 by weight; the concentration of the coating solution was 10 wt % and the coating material was cellulose acetate phthalate (CAP).
  • CAP cellulose acetate phthalate
  • CSMDP was prepared by the following steps:
  • API powder of Compound Salvia Militiorrhiza was added with water and stirred at 80° C. for 10 min or longer to obtain a pre-mixed API of Compound Salvia Militiorrhiza.
  • Material melting step the mixture of PEG-4000:PEG-6000 (1:1) and the pre-mixed API of Compound Salvia Militiorrhiza were charged into a homogenizer to homogenize at 2500 rpm for 100 min to give a material; the material was molten homogenously at 6000 rpm for 80 min; during the melting process, the temperature of the material was kept at 80° C. to obtain a molten medicine liquid;
  • Step (2) the molten medicine liquid was delivered to a dripper and dropped by means of vibration dropping at a dripper temperature of 100° C. and a vibration frequency of 200 Hz under a dropping pressure of 3.0 Bar and a acceleration speed of 20G and a dropping rate of 40 Kg/h; the dropping rate was matched with the melting rate in Step (1);
  • the resultant drop pills were dried by a gradient-rising temperature drying method, fluidized at 30° C., dried at 35° C. for 120 min, at 55° C. for 60 min and at 100° C. for 60 min to give dried uncoated drop pills; and,
  • Coating step the resultant dried uncoated drop pills were coated at 35° C. in a fluidized bed to obtain coated drop pills; the ratio of the coating material to the dried uncoated drop pills was 1:25 by weight; the concentration of the coating solution was 10 wt % and the coating material was methyl acrylate.
  • CSMDP was prepared by the following steps:
  • Material melting step the xylitol was firstly charged into a melting tank and heated to 90° C. to pre-melt, into which the API of Compound Salvia Militiorrhiza was charged and well mixed to give a molten medicine liquid;
  • Drying & coating step the resultant solid drop pills were dried in a fluidized state and drug-loading coated to give coated micro drop pills with a particle size of 0.2 mm ⁇ 1.0 mm; the drying temperature was 75° C.; and,
  • Packaging step the coated micro drop pills with a particle size of 0.2 mm ⁇ 1.0 mm were loaded into capsules; 100% of the capsules were on-line checkweighed with a capsule checkweigher and packaged to give the final product.
  • the formation of drop pills was measured visually by using a stroboscopic illumination to perform real-time monitoring and adjustment.
  • the steps of screening and regulating the drop pills could be added.
  • CSMDP was prepared by the following steps:
  • Material melting step the mixture of PEG-6000 and PEG-4000 was firstly charged into a melting tank and pre-molten by heating to 120° C., into which the API of Compound Salvia Militiorrhiza was charged and well mixed to give a molten medicine liquid;
  • Drying & coating step the resultant solid drop pills were dried in a fluidized state and drug-loading coated to give coated micro drop pills with a particle size of 0.5 mm ⁇ 1.0 mm; the drying temperature was 150° C.; and,
  • Packaging step the micro drop pills were loaded into capsules; 100% of the capsules were on-line checkweighed with a capsule checkweigher and packaged to give the final product.
  • the formation of drop pills was measured visually by using a stroboscopic illumination to perform real-time monitoring and adjustment.
  • the step of screening and regulating the drop pills could be added.
  • CSMDP was prepared by the following steps:
  • Material melting step the PEG-1000 was firstly charged into a melting tank and pre-molten by heating to 40° C., into which the API of Compound Salvia Militiorrhiza was charged and well mixed to give a molten medicine liquid;
  • Drying & coating step the resultant solid drop pills were dried in a fluidized state and drug-loading coated, fluidized at 20° C., dried at 25° C. for 60 min, further dried at 45° C. for 30 min and at 55° C. for 30 min to give the coated micro drop pill with a particle size of 3.0 mm ⁇ 4.0 mm; and,
  • Packaging step the micro drop pills were loaded into capsules; 100% of the capsules were on-line checkweighed with a capsule checkweigher and packaged to give the final product.
  • the formation of drop pills was measured visually by using a stroboscopic illumination to perform real-time monitoring and adjustment.
  • the step of screening and regulating the drop pills could be added.
  • CSMDP was prepared by the following steps:
  • Material melting step the mixture of PEG-6000 and PEG-4000 was firstly charged into a melting tank and pre-molten by heating to 120° C., into which the API of Compound Salvia Militiorrhiza was charged into a homogenizer to homogenize at 1000 rpm for 1 min and molten homogenously at 3000 rpm for 1 min, during the melting process, the temperature of the material was kept at 60° C. to obtain a molten medicine liquid;
  • Drying & coating step the resultant solid drop pills were dried in a fluidized state and drug-loading coated to give coated micro drop pills with a particle size of 0.2 mm; the drying temperature was 150° C.; and,
  • Packaging step the micro drop pills were loaded into capsules; 100% of the capsules were on-line checkweighed with a capsule checkweigher and packaged to give the final product.
  • CSMDP was prepared by the following steps:
  • Material melting step the PEG-6000 was firstly charged into a melting tank and pre-molten by heating to 120° C., into which the API of Compound Salvia Militiorrhiza was charged into a homogenizer to homogenize at 5000 rpm for 200 min and molten homogenously at 10000 rpm for 1 min, during the melting process, the temperature of the material was kept at 100° C. to obtain a molten medicine liquid;
  • Drying & coating step the resultant solid drop pills were dried in a fluidized state and drug-loading coated to give coated micro drop pills with a particle size of 4.0 mm; the drying temperature was 150° C.; and,
  • Packaging step the micro drop pills were loaded into capsules; 100% of the capsules were on-line checkweighed with a capsule checkweigher and packaged to give the final product.
  • CSMDP was prepared by the following steps:
  • Material melting step the PEG-4000 was firstly charged into a melting tank and pre-molten by heating to 120° C., into which the API of Compound Salvia Militiorrhiza was charged, homogenized at 3000 rpm for 10 min and molten homogenously at 4000 rpm for 5 min, during the melting process, the temperature of the material was kept at 70 ⁇ 90° C. to obtain a molten medicine liquid;
  • CSMDP was prepared by the following steps:
  • Material melting step the PEG-4000 was firstly charged into a melting tank and pre-molten by heating to 120° C., into which the API of Compound Salvia Militiorrhiza was charged, homogenized at 4000 rpm for 60 min and molten homogenously at 9000 rpm for 30 min, during the melting process, the temperature of the material was kept at 90° C. to obtain a molten medicine liquid;
  • CSMDP was prepared by the following steps:
  • Material melting step the PEG-6000 was firstly charged into a melting tank and pre-molten by heating to 90° C., into which the API of Compound Salvia Militiorrhiza was charged and well mixed to give a molten medicine liquid;
  • Drying & coating step the resultant solid drop pills were dried in a fluidized state and drug-loading coated to give coated micro drop pills with a particle size of 1.0 mm ⁇ 2.0 mm; the drying temperature was 75° C.; and,
  • Packaging step the coated micro drop pills were loaded into capsules; 100% of the capsules were on-line checkweighed with a capsule checkweigher and packaged to give the final product.
  • the formation of drop pills was measured visually by using a stroboscopic illumination to perform real-time monitoring and adjustment.
  • the step of screening and regulating the drop pills could be added.
  • the CSMDP prepared by the methods disclosed in the CSMDP PREPARATIVE EXAMPLES 2 ⁇ 17 had the similar merits such as high bioavailability, reduced administration dosage and good compliance to the patients. Meanwhile, the CSMDP prepared by the methods disclosed in CSMDP PREPARATIVE EXAMPLE 2 ⁇ 17 had the same merits listed in Table 2.
  • Qishenyiqi drop pill is a TCM preparation prepared by Astragalus membranaceus, Salvia Militiorrhiza, Panax Notoginseng and volatile oil from Lignum Dalbergiae Odoriferae. It is capable of significantly improving symptoms such as myocardial injury and heart dysfunction, which has been used clinically for treating diseases of chronic heart failure, myocarditis and its sequelae, myocardial infarction recovery stage and myocardial fibrosis.
  • the current Qishenyiqi drop pill has the merits such as small dosage, convenient administration, rapid dissolution, direct absorption into blood by mucosa, high bioavailability and high efficacy with no gastrointestinal stimulation and no obvious toxic and side effects.
  • the preparation method for QMDP known in the prior art mainly comprises the following steps: firstly, the following crude drugs were prepared: Astragalus membranaceus, Salvia Militiorrhiza, Panax Notoginseng , volatile oil from Lignum Dalbergiae Odoriferae and PEG-6000; Salvia Militiorrhiza and Panax Notoginseng were decocted with water and precipitated with ethanol; the ethanol was recovered and concentrated to obtain the Salvia Militiorrhiza and Panax Notoginseng extract; Astragalus membranaceus was decocted with water and precipitated with ethanol to obtain deposit of Astragalus membranaceus ; Lignum Dalbergiae Odoriferae was extracted with water to obtain volatile oil from Lignum Dalbergiae Odoriferae; the Salvia Militiorrhiza and Panax Notoginseng extract, the deposit of Astragalus membranaceus and PEG-6000 were well mol
  • Qishenyiqi micro drop pills are prepared by the API and the drop pill matrix in a ratio of 1:5 ⁇ 5:1 by weight.
  • the API is prepared by the following crude drugs by weight parts:
  • the API is prepared by the following crude drugs by weight parts:
  • the API is prepared by the following crude drugs by weight parts:
  • the micro drop pills are prepared by the API and the drop pill matrix in a ratio of 1:3 ⁇ 3:1 by weight, most preferably 1:(1 ⁇ 3) by weight.
  • the API of Qishenyiqi micro drop pill is used as the active pharmaceutical ingredient, which is prepared by the following steps: Astragalus membranaceus, Salvia Militiorrhiza and Panax Notoginseng were extracted and followed by addition of volatile oil from Lignum Dalbergiae Odoriferae.
  • the preparation of the API belongs to the prior art, and the API can be prepared by the conventional methods with the crude drugs in the ratios of the present invention, or by the commercially available Astragalus membranaceus extract, Salvia Militiorrhiza extract, Panax Notoginseng extract and volatile oil from Lignum Dalbergiae Odoriferae.
  • the API is preferably prepared by the following method:
  • Step (1) under an alkaline condition, Salvia Militiorrhiza and Panax Notoginseng are decocted with water for 1 ⁇ 3 times, 1 ⁇ 3 hours each time to give a decoction, and the decoction was filtered to get a filtrate; the filtrate is concentrated to give a concentrated liquid, into which 70 ⁇ 100% (v/v) ethanol is added to make the final concentration of ethanol 50 ⁇ 70% (v/v) and allow to stand still to get a supernatant; the supernatant is taken, filtered, ethanol is recovered and concentrated to give the Salvia Militiorrhiza and Panax Notoginseng extract.
  • Salvia Militiorrhiza and Panax Notoginseng are decocted with water and an appropriate amount of alkali for 2 times, 2 hours each time and filtered to get a filtrate for each decoction; the filtrates are combined and concentrated to give a concentrated liquid with a relative density of 1.13 ⁇ 1.23 (80° C.), into which ethanol is added to make a final concentration of ethanol 65 ⁇ 70% (v/v) and allow to stand still for 12 hours or longer to get a supernatant; the supernatant is filtered, ethanol is recovered and concentrated to give the Salvia Militiorrhiza and Panax Notoginseng extract with a relative density of 1.30 ⁇ 1.38 (80° C.).
  • Step (2) Astragalus membranaceus is decocted with an alkaline aqueous solution for 1 ⁇ 3 times, 1 ⁇ 3 hours each time, to give a decoction; the decoction is filtered to give Filtrate I; dregs of the decoction is further decocted with water for 1 ⁇ 3 times, 1 ⁇ 3 hours each time, to give a decoction; the decoction is filtered to give Filtrate II; Filtrate I and Filtrate II are combined and concentrated to give a concentrated liquid, into which 50 ⁇ 100% (v/v) ethanol is added to perform ethanol precipitation for 1 ⁇ 3 times to make the final concentration of ethanol 60 ⁇ 80% (v/v) and allow to stand still to get a supernatant; the supernatant is filtered to give Filtrate III; Filtrate III is recovered and concentrated by ethanol to give the Astragalus membranaceus extract.
  • Step (2) Astragalus membranaceus is decocted with water and an appropriate amount of sodium bicarbonate for 2 hours to give a decoction; the decoction was filtered to give Filtrate I; dregs of the decoction is further decocted with water for 1 hour to give a decoction; the decoction is filtered to give Filtrate II; Filtrate I and Filtrate II are combined and concentrated to give a concentrated liquid with a relative density 1.05 ⁇ 1.20 (75 ⁇ 5° C.), ethanol is added into the concentrated liquid to make the final concentration of ethanol 60 ⁇ 1% (v/v) and allow to stand still for 12 hours or longer to get a supernatant, the supernatant is filtered and recovered ethanol under a reduced pressure to obtain a concentrated liquid with a relative density of 1.18 ⁇ 1.30 (60 ⁇ 5° C.), into which ethanol is added to make the final concentration of ethanol 80 ⁇ 1% (v/v) and allow to stand still for 12 hours
  • the alkaline condition is at a pH value of 7.5 ⁇ 9.0 and the alkali is, but not limited to, selected from the group consisting of sodium bicarbonate, sodium carbonate, disodium hydrogen phosphate, sodium dihydrogen phosphate, sodium hydroxide, potassium hydroxide and magnesium hydroxide.
  • the preparation method for preparing the QMDP comprises the following steps:
  • Material melting step charging the API and the drop pill matrix in a ratio of 1:5 ⁇ 5:1 by weight into a homogenizer, mixing homogenously at 1000 ⁇ 5000 rpm for 1 ⁇ 200 min, melting homogenously at 3000 ⁇ 10000 rpm for 1 ⁇ 100 min; during the melting process, the temperature of the material is kept at 60 ⁇ 100° C. to obtain a molten medicine liquid;
  • Step (2) Dropping step: delivering the molten medicine liquid to a dripper at 70° C. ⁇ 300° C., and acquiring medicine drops by means of vibration dropping at a vibration frequency of 50 ⁇ 300 Hz under a dropping pressure of 0.5 ⁇ 4.0 Bar; the dropping rate is matched with the melting rate in Step (1);
  • Step (2) and Step (3) the pill weight decreased from 23.5 ⁇ 27.5 mg of the traditional drop pills to 3 ⁇ 5 mg, which can be loaded into capsules; the use of gas cooling can solve the problems such as residual coolant of liquid paraffin in the current drop pills.
  • the following materials were prepared: 80 g of the API of QMDP and 165 g of PEG-6000.
  • Pre-mixing step the API of QMDP was added with water to pre-mix, stirred in a heat-insulated tank at 40 ⁇ 10° C. for 60 min or longer to make the water content of API of QMDP at 13.0 wt % to give a pre-mixed API of QMDP for later use;
  • Drying step the resultant drop pills were dried in a fluidized state; until the drop pills reached a better fluidization state in the bed of the fluidized bed, the temperature was increased to 25° C. to dry for 60 min, further increased to 45° C. to dry for 30 min, continuously increased to 55° C. to dry for 30 min, and deceased 30° C. or lower to discharge to give uncoated drop pills as a intermediate product, and the water content of the uncoated drop pills was controlled in a range of 3.0 ⁇ 7.0 wt %;
  • Coating step the amount of coating powder was calculated based on the coating feed capacity and formulation; Opadry, which has 4 wt % of the weight of the uncoated drop pills, was used to prepare a 18 wt % coating solution and stirred for 45 min; the inlet air temperature was initially set to 25° C.; after the qualified uncoated drop pills were loaded into the fluidized bed, the inlet air temperature was increased to 48° C.; until the temperature of the drop pills was up to 38° C., the coating was started; the temperature of the material was kept in the range of 35 ⁇ 45° C. during the coating and decreased 30° C.
  • the drop pills were discharged, screened to give coated drop pills as a intermediate product, the coating weigh of the coated drop pills was controlled in a range of 3.3 ⁇ 0.7% and the water content was controlled in a range of 3.0 ⁇ 7.0 wt %; and,
  • the formation of the drop pills was measured visually by using a stroboscopic illumination to perform a real-time monitoring and adjustment.
  • the steps of screening and regulating the drop pills could be added.
  • API of QMDP was prepared by the following method:
  • Step (1) Salvia Militiorrhiza and Panax Notoginseng were decocted with water and an appropriate amount of alkali for 2 times, 2 hours each time to give a decoction, and the decoction was filtered to get filtrates; the filtrates were combined and concentrated to give a concentrated liquid with a relative density of 1.13 ⁇ 1.23(80° C.); ethanol was added into the concentrated liquid to make a final concentration of ethanol 65 ⁇ 70% (v/v) and allowed to stand still for 12 hours or longer to get a supernatant; the supernatant was filtered, and the ethanol therein was recovered and concentrated to give the Salvia Militiorrhiza and Panax Notoginseng extract with a relative density of 1.30 ⁇ 1.38(80° C.).
  • Step (2) Astragalus membranaceus is decocted with water and an appropriate amount of sodium bicarbonate for 2 hours to give a decoction; the decoction was filtered to give Filtrate I; dregs of the decoction is further decocted with water for 1 hour to give a decoction; the decoction is filtered to give Filtrate II; Filtrate I and Filtrate II are combined and concentrated to give a concentrated liquid with a relative density 1.05 ⁇ 1.20 (75 ⁇ 5° C.), ethanol is added into the concentrated liquid to make the final concentration of ethanol 60 ⁇ 1% (v/v) and allow to stand still for 12 hours or longer to get a supernatant, the supernatant is filtered and recovered ethanol under a reduced pressure to obtain a concentrated liquid with a relative density of 1.18 ⁇ 1.30 (60 ⁇ 5° C.), into which ethanol is added to make the final concentration of ethanol 80 ⁇ 1% (v/v) and allow to stand still for 12 hours or
  • the following materials were prepared: 100 g of Salvia Militiorrhiza and Panax Notoginseng extract, 200 g of Astragalus membranaceus extract, 10 g of volatile oil from Lignum Dalbergiae Odoriferae and 900 g of PEG-6000 as the drop pill matrix.
  • Material melting step the PEG-6000 was loaded into a melting tank and pre-molten by heating to 70 ⁇ 80° C., into which a uniform mixture of the Salvia Militiorrhiza and Panax Notoginseng extract and the Astragalus membranaceus extract as well as volatile oil from Lignum Dalbergiae Odoriferae were added, mixed and homogenized to give a molten medicine liquid;
  • Step (2) Dropping step: the molten medicine liquid was delivered to a dripper and dropped by means of vibration dropping at a dripper temperature of 80° C. and a vibration frequency of 50 Hz; the dropping rate was matched with the melting rate in Step (1); and,
  • Drying & coating step the resultant drop pills was dried in a fluidized state and drug-loading coated at 150° C., screened, regulated and packaged to obtain the final product.
  • the API of QMDP was prepared by the following crude drugs by weight parts: Astragalus membranaceus 100 parts, Salvia Militiorrhiza 50 parts, Panax Notoginseng 10 parts, volatile oil from Lignum Dalbergiae Odoriferae 0.5 parts, and the ratio of the API of QMDP to PEG-6000 was 1:5 by weight, the Qishenyiqi micro drop pills were prepared by the same method as QMDP PREPARATIVE EXAMPLE 1.
  • the API of QMDP was prepared by the following crude drugs by weight parts: Astragalus membranaceus 200 parts, Salvia Militiorrhiza 100 parts, Panax Notoginseng 20 parts, volatile oil from Lignum Dalbergiae Odoriferae 2 parts, and the ratio of the API of QMDP to PEG-6000 was 5:1 by weight, the Qishenyiqi micro drop pills were prepared by the same method as QMDP PREPARATIVE EXAMPLE 1.
  • the following materials were prepared: 80 g of the API of QMDP, 165 g of a cyclodextrin and agar (1:1) mixture.
  • the QMDP was prepared by the following method:
  • Material melting step the cyclodextrin and agar (1:1) mixture was charged into a homogenizer with the API of QMDP to homogenize at 1000 rpm for 1 min to give a material; the material was molten homogenously at 3000 rpm for 1 min; during the melting process, the temperature of the material was kept at 60° C. to obtain a molten medicine liquid;
  • Step (2) the molten medicine liquid was delivered to a dripper and dropped by means of vibration dropping at a dripper temperature of 70° C. and a vibration frequency of 50 Hz under a dropping pressure of 0.5 Bar; the dropping rate was matched with the melting rate in Step (1); and,
  • the following materials were prepared: 80 g of the API of QMDP, 165 g of arabic gum and lactose (1:1) mixture.
  • the QMDP was prepared by the following method:
  • Material melting step the arabic gum and lactose (1:1) mixture was charged into a homogenizer with the API of QMDP to homogenize at 5000 rpm for 200 min to give a material; the material was molten homogenously at 10000 rpm for 100 min; during the melting process, the temperature of the material was kept at 100° C. to obtain a molten medicine liquid;
  • Step (2) the molten medicine liquid was delivered to a dripper and dropped by means of vibration dropping at a dripper temperature of 300° C. and a vibration frequency of 300 Hz under a dropping pressure of 4.0 Bar; the dropping rate was matched with the melting rate in Step (1); and,
  • the following materials were prepared: 80 g of the API of QMDP and 165 g of lactitol.
  • the QMDP was prepared by the following method:
  • Material melting step the API of QMDP and lactitol were loaded into a homogenizer to homogenize at 2500 rpm for 100 min and molten homogenously at 6000 rpm for 50 min to give a molten medicine liquid; during the melting process, the temperature of the material was kept at 80° C.;
  • Step (2) the molten medicine liquid was delivered to a dripper and dropped by means of vibration dropping at a dripper temperature of 150° C. and a vibration frequency of 150 Hz under a dropping pressure of 2 Bar; the dropping rate was matched with the melting rate in Step (1); and,
  • Coating step the uncoated drop pills were coated at 45° C. on a fluidized bed to give coated drop pills, the ratio of the coating material of shellac to the uncoated drop pills was 1:25 by weight, the coating solution is at 10 wt %.
  • the following materials were prepared: 80 g of the API of QMDP powder and 165 g of PEG-8000.
  • the QMDP was prepared by the following method:
  • the API of QMDP powder was added with water and stirred at 60° C. for 10 min or longer to give a pre-mixed material.
  • Material melting step the pre-mixed material and PEG-8000 were loaded into a homogenizer to homogenize at 2500 rpm for 100 min and molten homogenously at 6000 rpm for 50 min to give a molten medicine liquid; during the melting process, the temperature of the material was kept at 80° C.;
  • Step (2) the molten medicine liquid was delivered to a dripper and dropped by means of vibration dropping at a dripper temperature of 150° C. and a vibration frequency of 150 Hz under a dropping pressure of 2 Bar; the dropping rate was matched with the melting rate in Step (1); and,
  • Coating step the dried uncoated drop pills were coated in a fluidized bed to coat at 35° C. to give coated drop pills; the ratio of the coating material of CAP to the uncoated drop pills was 1:25 by weight; the concentration of coating solution was 25 wt %.
  • the following materials were prepared: 90 g of the API of QMDP powder and 270 g of PEG-1000.
  • the QMDP was prepared by the following method:
  • the API of QMDP powder was added with water and stirred at 30° C. for 10 min or longer to give a pre-mixed material.
  • Material melting step the pre-mixed material and PEG-1000 were loaded into a homogenizer to homogenize at 2500 rpm for 100 min and molten homogenously at 6000 rpm for 20 min to give a molten medicine liquid; during the melting process, the temperature of the material was kept at 100° C.;
  • Step (2) the molten medicine liquid was delivered to a dripper and dropped by means of vibration dropping at a dripper temperature of 70° C., a vibration frequency of 100 Hz under a dropping pressure of 1.0 Bar, an acceleration speed of 1G and a dropping rate of 10 Kg/h, which was matched with the melting rate in Step (1);
  • the resultant drop pills were dried by a gradient-rising temperature drying method, fluidized at ⁇ 20° C., dried at 15° C. for 10 min, at 35° C. for 10 min and at 55° C. for 30 min to give dried uncoated drop pills; and,
  • Coating step the dried uncoated drop pills were coated in a fluidized bed at 40° C. to give coated drop pills; the ratio of the coating material of Opadry to the uncoated drop pill was 1:25 by weight; the concentration of coating solution was 20 wt %.
  • the following materials were prepared: 105 g of the API of QMDP powder and 35 g of a PEG-4000 and PEG-6000 (1:1) mixture.
  • the QMDP was prepared by the following method:
  • the API of QMDP powder was added with water and stirred at 80° C. for 10 min or longer to give a pre-mixed material.
  • Material melting step the pre-mixed material and the PEG-4000 and PEG-6000 (1:1) mixture were loaded into a homogenizer to homogenize at 2500 rpm for 100 min and molten homogenously at 6000 rpm for 80 min to give a molten medicine liquid; during the melting process, the temperature of the material was kept at 80° C.;
  • Step (2) the molten medicine liquid was delivered to a dripper and dropped by means of vibration dropping at a dripper temperature of 100° C., a vibration frequency of 200 Hz under a dropping pressure of 3.0 Bar, an acceleration speed of 20G and a dropping rate of 40 Kg/h, which was matched with the melting rate in Step (1);
  • the resultant drop pills were dried by a gradient-rising temperature drying method, fluidized at 30° C., dried at 35° C. for 120 min, at 55° C. for 60 min and at 100° C. for 60 min to give dried uncoated drop pills; and,
  • Coating step the dried uncoated drop pills were coated in a fluidized bed at 35° C. to give coated drop pills; the ratio of the coating material of methyl acrylate to the uncoated drop pills was 1:25 by weight; the concentration of coating solution was 5 wt %.
  • Salvia Militiorrhiza extract can either be prepared by the conventional methods or commercially available.
  • 600 g of the Salvia Militiorrhiza extract was added with water (60 g) and 600 g of PEG-6000, charged into a melting tank and totally molten and mixed to give a molten medicine liquid by heating to 90° C. ⁇ 100° C.
  • the molten medicine liquid was delivered under pressure to a dripper and dropped by means of vibration dropping at a dripper temperature of 80° C. ⁇ 100° C. and a vibration frequency of 150 Hz.
  • the drops were cooled with low-temperature nitrogen and the cooling temperature was ⁇ 140° C.
  • the drop pills were dried with a fluidized bed at 150° C. and coated with a coating solution (18 ⁇ 20 wt %), screened, regulated and packaged to give the final product.
  • Salvia Militiorrhiza extract can either be prepared by the conventional methods or commercially available.
  • the Huoxiangzhengqi extract can be prepared by the methods disclosed in Chinese patent applications CN 100563635A and CN 1745799A and patchouli oil and perilla leaf oil were commercially available.
  • Huoxiangzhengqi extract 200 g of Huoxiangzhengqi extract, 1 ml of patchouli oil, 2 ml of perilla leaf oil and 600 g of PEG-6000 were prepared. All of the Huoxiangzhengqi extract and 550 g of PEG-6000 was charged into 1# melting tank and molten by heating to 65 ⁇ 85° C. to give a uniform liquid. 1 ml of patchouli oil, 2 ml of perilla leaf oil and 50 g of PEG-6000 were charged into 2# melting tank and molten by heating to 65 ⁇ 85° C. to give a uniform liquid.
  • the liquid in 2# melting tank was delivered to the inner layer of a double-layer dripper and the liquid in 1# melting tank was delivered to the outer layer of the double-layer dripper.
  • the vibration frequency of the dripper was adjusted to 200 Hz.
  • the molten medicine liquid was flowed under pressure into the dripper and dropped by means of vibration dropping at a dripper temperature of 80° C.
  • the drops were cooled with low-temperature air to give solid drop pills.
  • the cooling temperature was ⁇ 40° C.
  • the Huoxiangzhengqi extract can be prepared by the methods disclosed in Chinese patent applications CN 100563635A and CN 1745799A and the patchouli oil and perilla leaf oil were commercially available.
  • CMC carboxymethyl cellulose
  • the CMC was charged into a melting tank and pre-molten by heating to 90 ⁇ 100° C., into which the andrographolide was added and mixed to give a uniform liquid.
  • the vibration frequency of a pneumatic dripper was adjusted to 30 Hz.
  • the temperature of the dripper was controlled at 80° C.
  • the molten medicine liquid was flowed under pressure into the dripper and dropped from the bottom of the dripper into a cooling duct.
  • the drops were cooled with low-temperature nitrogen to give solid drop pills.
  • the cooling temperature was ⁇ 20° C.
  • the drop pills were dried in a fluidized state and drug loading coated.
  • the drop pills were screened, regulated and packaged to obtain the final product with a particle size of drop pill of 1.5 mm ⁇ 2 mm.
  • the andrographolide was either prepared by the methods known in the prior art or commercially available.
  • the drop pills were dried in a fluidized state at 75° C. and drug loading coated to obtain drop pills with a particle size of 1.0 mm ⁇ 2.0 mm.
  • the drop pills were loaded into capsules, and 100% of the capsules were on-line checkweighed with a capsule checkweigher, packaged to give the final product.
  • Salvia Militiorrhiza and Ginkgo Biloba extract was prepared by the method of Chinese patent CN 1872099B.
  • the formation of drop pills was measured visually by using a stroboscopic illumination to perform real-time monitoring and adjustment.
  • the step of screening and regulating could be added.
  • the drop pills were dried in a fluidized state at 75° C. and drug loading coated to obtain drop pills with a particle size of 1.0 mm ⁇ 2.0 mm.
  • the drop pills were loaded into capsules, and 100% of the capsules were on-line checkweighed with a capsule checkweigher, packaged to give the final product.
  • Salvia Militiorrhiza and Ginkgo Biloba extract was prepared by the method of Chinese patent CN 101015527B.
  • the formation of drop pills was measured visually by using a stroboscopic illumination to perform real-time monitoring and adjustment.
  • the step of screening and regulating could be added.
  • the drops were cooled with low-temperature inert gas to give solid drop pills.
  • the cooling temperature was ⁇ 20° C.
  • the drop pills were dried in a fluidized state at 75° C. and drug loading coated to obtain drop pills with a particle size of 1.0 mm ⁇ 2.0 mm.
  • the drop pills were loaded into capsules, and 100% of the capsules were on-line checkweighed with a capsule checkweigher, packaged to give the final product.
  • the Salvia Militiorrhiza and Panax Notoginseng extract and volatile oil from Lignum Dalbergiae Odoriferae were commercially available.
  • the Salvia Militiorrhiza and Panax Notoginseng extract can be prepared by the method for preparing the Salvia Militiorrhiza and Panax Notoginseng extract in the preparation of the CSMDP or QMDP.
  • the formation of drop pills was measured visually by using a stroboscopic illumination to perform real-time monitoring and adjustment.
  • the step of screening and regulating could be added.
  • PNS Panax Notoginseng saponins
  • starch 400 g of Panax Notoginseng saponins (PNS) and 400 g of starch were prepared.
  • the starch was charged into a melting tank and pre-molten by heating to 70 ⁇ 80° C., into which the PNS was added and mixed to give a uniform liquid.
  • the vibration frequency of a pneumatic dripper was adjusted to 30 Hz.
  • the temperature of the dripper was controlled at 80° C.
  • the molten medicine liquid was flowed under pressure into the dripper that was heat-insulated by a steam jacket and dropped from the bottom of the dripper into a cooling duct.
  • the drops were cooled with low-temperature nitrogen to give solid drop pills.
  • the cooling temperature was ⁇ 20° C.
  • the drop pills were dried in a fluidized state, drug loading coated and packaged to obtain drop pills with a particle size of 0.5 mm ⁇ 1 mm.
  • micro drop pills prepared by the methods disclosed in EXAMPLES 3 ⁇ 8 had the same merits listed in Table 2.

Landscapes

  • Health & Medical Sciences (AREA)
  • Life Sciences & Earth Sciences (AREA)
  • Chemical & Material Sciences (AREA)
  • Medicinal Chemistry (AREA)
  • Veterinary Medicine (AREA)
  • General Health & Medical Sciences (AREA)
  • Public Health (AREA)
  • Animal Behavior & Ethology (AREA)
  • Pharmacology & Pharmacy (AREA)
  • Natural Medicines & Medicinal Plants (AREA)
  • Epidemiology (AREA)
  • Engineering & Computer Science (AREA)
  • Bioinformatics & Cheminformatics (AREA)
  • Botany (AREA)
  • Biotechnology (AREA)
  • Mycology (AREA)
  • Microbiology (AREA)
  • Medical Informatics (AREA)
  • Alternative & Traditional Medicine (AREA)
  • Zoology (AREA)
  • General Chemical & Material Sciences (AREA)
  • Organic Chemistry (AREA)
  • Chemical Kinetics & Catalysis (AREA)
  • Nuclear Medicine, Radiotherapy & Molecular Imaging (AREA)
  • Heart & Thoracic Surgery (AREA)
  • Cardiology (AREA)
  • Diabetes (AREA)
  • Vascular Medicine (AREA)
  • Urology & Nephrology (AREA)
  • Hematology (AREA)
  • Medicinal Preparation (AREA)
  • Medicines Containing Plant Substances (AREA)
  • Pharmaceuticals Containing Other Organic And Inorganic Compounds (AREA)

Abstract

The present invention relates to a preparation method for a traditional Chinese medicine drop pill and a traditional Chinese medicine micro drop pill prepared by using the method, and in particular, the present invention relates to a micro drop pill preparation method with high drug-loading capacity, simple preparation process and high production rate and a micro drop pill prepared by using the method. Specially, The drop pill preparation method used comprises the following steps: (1) material melting step: heat melting a medicine and a drop pill matrix to obtain a molten medicine liquid; (2) dropping step: delivering the molten medicine liquid to a dripper, and acquiring medicine drops of the molten medicine liquid by means of vibration dropping; and, (3) condensation step: cooling the medicine drops with a cooling gas to obtain micro drop pills.

Description

    CROSS REFERENCE TO RELATED APPLICATIONS
  • This is a continuation of U.S. patent application Ser. No. 14/903,896, filed Jan. 8, 2016, which is the National Stage of International Application No. PCT/CN2014/082104, filed Jul. 11, 2014, which claims priority to Chinese Application No. 201310290966.9, filed Jul. 11, 2013, Chinese Application No. 201310290967.3, filed Jul. 11, 2013, Chinese Application No. 201310290968.8, filed Jul. 11, 2013 and Chinese Application No. 201310291465.2, filed Jul. 11, 2013.
    • FIELD OF THE INVENTION
  • The present invention relates to a formulation of a micro drop pill and the preparation method thereof, more particularly, the present invention relates to a micro drop pill preparation method with high drug-loading capacity, simple preparation process and high production rate and a formulation of micro drop pill prepared by the method. The method can be used to prepare an uncoated micro drop pill, a coated micro drop pill and a micro drop pill capsule with high drug-loading capacities.
    • BACKGROUND OF THE INVENTION
  • Drop pill, as an important traditional Chinese medicine preparation, has been used widely. In practice, it has the following merits: shortened production cycle, dust pollution-free, high bioavailability, rapid onset of effect, prolonged action in topical administration, reduced volatility of drug, increased drug stability and being easily carried and stored.
  • However, the preparation method of the traditional drop pill is to drop a molten medicine liquid into an immiscible cooling medium (in most cases, a coolant is used as the cooling medium) to give the drop pill. Because the drop pill is formed mainly by factors of freely-falling gravity, surface tension of medicine liquid and internal stress, the unit drug-loading capacity is small (usually, the drug-loading capacity of the active pharmaceutical ingredient (API) is only about 25 wt %) and the amount of matrix used is very large. This cannot meet the requirement of international market that the maximum daily dosage of polyethylene glycols (PEGs) matrix should not exceed 700 mg. Moreover, it is difficult to prepare the traditional drop pill with a diameter of less than 2.5 mm, so the patients have to take a lot of hard-to-swallow pills each time, which will not satisfy fast-paced trend of modern life, and be prone to the problem of inaccurate dosage. Thus, it is generally unacceptable by the international consumers. In addition, there are a number of shortcomings in the preparation of the traditional drop pills, e.g. low dropping frequency, poor roundness, and a large variation in the pill weight and the particle size of the drop pills. Because the coolant has been used for solidifying the drop pills, the necessary step is needed in the subsequent process to remove the coolant, and the irremovable coolant may cause the problem of residual organic solvent. Besides, drying methods for the traditional drop pill have the defects of prolonged time, uneven drying and easily leading to evaporation of volatile oil-containing products and precipitation of borneol of borneol-containing products during drying.
  • As a result, how to obtain a micro drop pill with high production rate, reduced amount of matrix, increased drug-loading capacity and smaller particle size is an important subject for the development and exploration of the modern preparation process of the drop pill.
    • SUMMARY OF THE INVENTION
  • The objective of the present invention is to provide a simple and high-speed preparation method to prepare a micro drop pill with high drug-loading capacity and small amount of matrix. The preparation method for preparing the micro drop pill comprises the following steps:
  • (1) Material melting step: heat melting a medicine and a drop pill matrix to obtain a molten medicine liquid;
  • (2) Dropping step: delivering the molten medicine liquid under pressure to a dripper, and acquiring medicine drops of the molten medicine liquid by means of vibration dropping; and,
  • (3) Condensation step: cooling the medicine drops with a cooling gas to obtain micro drop pills.
  • Another objective of the present invention is to provide a TCM formulation of micro drop pill. In the micro drop pill, the ratio of the medicine to the drop pill matrix is 1:5˜5:1 by weight, and the particle size of the micro drop pill is 0.2 mm˜4 mm. Moreover, the micro drop pill is prepared according to the preparation method of the micro drop pill of the present invention, and there is no residual coolant.
  • In the present invention, the micro drop pill means that the micro drop pill has a smaller particle size compared with the traditional drop pill. More specifically, the micro drop pill refers to the one with a particle size of 0.2 mm˜4 mm, especially, the one with a particle size of 0.2 mm˜2 mm, preferably 1 mm˜2 mm.
  • In the present invention, the coolant of the drop pill means the coolant commonly-used in the preparation of the traditional drop pill, for example, but not limited to, liquid paraffin, methyl silicone oil and plant oil (soybean oil and castor oil etc.).
  • In the present invention, the medicine includes any one of TCMs or chemicals that is suitable to be prepared into the drop pills. In terms of the TCMs, the extract is preferred to be used, e.g. Ginkgo Biloba extract, Bupleurum extract, Salvia Militiorrhiza extract and Andrographis Paniculata extract, as well as the extracts of Qishenyiqi, Huoxiangzhengqi and Compound Salvia Militiorrhiza. These extracts can either be commercially available, or prepared by the method known in the prior art. In the present invention, the micro drop pill includes, but is not limited to: Compound Salvia Militiorrhiza micro drop pill (CSMDP), Qishenyiqi micro drop pill (QMDP), Salvia Militiorrhiza micro drop pill (SMDP), Huoxiangzhengqi micro drop pill (HMDP), Andrographis Paniculata micro drop pill (AMDP), Compound Ginkgo Biloba micro drop pill (CGMDP), Guanxindanshen micro drop pill (GMDP) and Xuesaitong micro drop pill (XMDP) etc. Preferably, the medicines in the present invention are the API of Compound Salvia Militiorrhiza and the API of Qishenyiqi.
  • Another objective of the present invention is to provide Compound Salvia Militiorrhiza micro drop pill prepared by the method of the present invention, characterized in that the ratio of the API of Compound Salvia Militiorrhiza to the drop pill matrix is 1:5˜5:1 by weight, and a particle size of the micro drop pill is 0.2 mm˜4 mm, preferably 0.2 mm˜2 mm, more preferably 1 mm˜2 mm. The API of Compound Salvia Militiorrhiza is prepared with the following crude drugs by weight parts: Salvia Militiorrhiza 75.0˜90.0 parts, Panax Notoginseng 10.0˜25.0 parts and borneol 0.1˜4.0 parts, and is prepared by the preparation method for the micro drop pill of the present invention. There is no residual coolant in the micro drop pills.
  • Another objective of the present invention is to provide QMDP (Qishenyiqi micro drop pill) prepared by the method of the present invention, characterized in that the ratio of the API of Qishenyiqi to the drop pill matrix is 1:5˜5:1 by weight, and the particle size 0.2 mm˜4 mm, preferably 0.2 mm˜2 mm, more preferably 1 mm˜2 mm. The API of Qishenyiqi is prepared by the following crude drugs by weight parts: Astragalus membranaceus 100˜200 parts, Salvia Militiorrhiza 50˜100 parts, Panax Notoginseng 10˜20 parts and volatile oil from Lignum Dalbergiae Odoriferae 0.5˜2 parts, and is prepared by the preparation method for the micro drop pill of the present invention. There is no residual coolant in the micro drop pills.
  • More specifically, as the first aspect of the invention, the present invention is achieved by the following technical solutions:
  • 1. A preparation method for a micro drop pill comprising the following steps:
  • (1) Material melting step: heat melting a medicine and a drop pill matrix to obtain a molten medicine liquid;
  • (2) Dropping step: delivering the molten medicine liquid under pressure to a dripper, and acquiring medicine drops of the molten medicine liquid by means of vibration dropping; and,
  • (3) Condensation step: cooling the medicine drops with a cooling gas to obtain micro drop pills.
  • 2. The preparation method according to the 1st paragraph, wherein the method comprises the following steps:
  • (1) Material melting step: heat melting the medicine and the drop pill matrix at 40° C.˜−120° C., homogenizing for 0.5˜4 hours to obtain a homogenized molten medicine liquid, and the ratio of the medicine to the drop pill matrix is 1:5˜5:1 by weight;
  • (2) Dropping step: delivering the molten medicine liquid under pressure to the dripper, and acquiring medicine drops at a vibration frequency for dropping of 20˜300 Hz under a dropping pressure of 0.5˜4.0 Bar, a temperature of the dripper of 40° C.˜−200° C. and a viscosity of the molten medicine liquid of 300˜1500 cp; and,
  • (3) Condensation step: cooling the medicine drops with a cooling gas for forming by solidifying, obtaining micro drop pills having a particle size of 0.2 mm˜4 mm, the temperature of the cooling gas is 0° C. or lower.
  • 3. The preparation method according to the 1st or 2nd paragraph, wherein in Step (1), the drop pill matrix includes one or more selected from the group consisting of PEGs, sorbitol, xylitol, lactitol, maltose, starch, methylcellulose, sodium carboxymethyl cellulose, hydroxypropyl methylcellulose (HPMC), arabic gum, alginic acid, dextrin, cyclodextrin, agar and lactose; preferably solid PEGs, such as PEG-1000, PEG-2000, PEG-3000, PEG-4000, PEG-5000, PEG-6000, PEG-7000 and PEG-8000; more preferably one or more selected from the group consisting of PEG-1000, PEG-2000, PEG-3000, PEG-4000, PEG-6000 and PEG-8000; most preferably PEG-6000, PEG-4000 or the combination of PEG-4000 and PEG-6000.
  • 4. The preparation method according to any one of the 1st˜3rd paragraphs, wherein in Step (1), the temperature for heat melting is at 60˜100° C., more preferably at 65˜90° C., further preferably 75˜85° C.
  • 5. The preparation method according to any one of the 2nd˜4th paragraphs, wherein in Step (1), the homogenizing time preferably is 1˜3 hours, further preferably 2 hours.
  • 6. The preparation method according to any one of the 1st˜5th paragraphs, wherein in Step (1), the ratio of the medicine to the drop pill matrix is 1:3˜3:1 by weight, preferably 1:(1˜3) by weight.
  • 7. The preparation method according to any one of the 1st˜6th paragraphs, wherein in Step (2), the temperature of the dripper is at 40˜120° C., preferably at 40˜100° C.; the vibration frequency for dropping is preferably at 20˜300 Hz, more preferably 50˜300 Hz, more preferably 20˜200 Hz, more preferably 20˜150 Hz, most preferably 50˜150 Hz; the vibration mode includes magnetic/electronic vibration or pneumatic vibration.
  • 8. The preparation method according to any one of the 1st˜7th paragraphs, wherein in Step (3), the temperature of the cooling gas is at 0° C.˜−150° C., preferably −10˜−140° C., further preferably −40° C.˜−140° C., further preferably −60° C.˜−140° C., most preferably −80° C.˜−120° C.; and the cooling gas is air, nitrogen or inert gas.
  • 9. The preparation method according to any one of the 1st˜8th paragraphs, wherein in Step (3), the particle size of the micro drop pill is 1.0 mm˜2.0 mm, preferably 0.5 mm˜2 mm.
  • 10. The preparation method according to the 2nd paragraph comprising the following steps:
  • (1) Material melting step: heat melting the medicine and the drop pill matrix at 60° C.˜100° C., homogenizing for 1˜3 hours to obtain a homogenized molten medicine liquid, the ratio of the medicine to the drop pill matrix is 1:3˜3:1 by weight;
  • (2) Dropping step: delivering the molten medicine liquid under pressure to a dripper, and acquiring medicine drops at a vibration frequency for dropping of 20˜200 Hz under a dropping pressure of 0.5˜4.0 Bar, the temperature of the dripper of 60° C.˜−120° C. and a viscosity of the molten medicine liquid of 700˜1000 cp; and,
  • (3) Condensation step: cooling the medicine drops with a cooling gas for forming by solidifying, obtaining the micro drop pills having a particle size of 0.5 mm˜2 mm, the temperature of the cooling gas is 0° C.˜−150° C.
  • 11. The preparation method according to the 2nd paragraph comprising the following steps:
  • (1) Material melting step: charging the medicine and the drop pill matrix into a homogenizer, mixing homogenously at 1000˜5000 rpm for 1˜200 min, then melting homogenously at 3000˜10000 rpm for 1˜100 min; during the melting process, the temperature is kept at 60˜100° C. to obtain the molten medicine liquid; the ratio of the medicine to the drop pill matrix is 1:5˜5:1 by weight;
  • (2) Dropping step: delivering the molten medicine liquid under pressure to the dripper, and acquiring medicine drops from the dripper by means of vibration dropping at a vibration frequency of 20˜300 Hz under a dropping pressure of 0.5˜4.0 Bar and the temperature of the dripper of 40° C.˜−200° C., the dropping rate is matched with the melting rate in Step (1); and
  • (3) Condensation step: cooling the medicine drops with a cooling gas rapidly to solidify, and obtaining solid drop pills having a particle size of 0.2 mm˜4.0 mm; the temperature of the cooling gas is 0° C.˜−150° C.
  • 12. The preparation method according to the 11th paragraph, wherein in Step (1), the ratio of the medicine to the drop pill matrix is 1:3˜3:1 by weight, mixing homogeneously at 3000˜5000 rpm for 10˜60 min, then melting homogeneously at 4000˜9000 rpm for 5˜30 min, during the melting process, the temperature is kept at 70˜90° C.
  • 13. The preparation method according to the 11th paragraph, wherein in Step (1), the ratio of the medicine to the drop pill matrix is 1:(1˜3) by weight, mixing homogeneously at 3000˜4000 rpm for 10˜30 min, then melting homogeneously at 4000˜6000 rpm for 6˜30 min, during the melting process, the temperature is kept at 75˜85° C.
  • 14. The preparation method according to the 11th paragraph, wherein in Step (2), the temperature of the dripper is at 70˜100° C., the vibration frequency for dropping is at 90˜200 Hz, the dropping pressure is at 1.0˜3.0 Bar; preferably the vibration frequency is at 137 Hz, an acceleration speed is at 4G, the dropping pressure is at 1.8 Bar and the temperature of the dripper is at 75˜85° C.
  • 15. The preparation method according to the 11th paragraph, in Step (2), the dropping rate is 10˜40 Kg/h, preferably 12˜30 Kg/h, further preferably 15˜25 Kg/h.
  • 16. The preparation method according to any one of the 1st˜15th paragraphs, wherein the method additionally comprises a drying step as Step (4): drying the low-temperature drop pills from Step (3) on a fluidized-bed at 40˜150° C., preferably at 40˜60° C. for 1˜4 hours, preferably 1˜3 hours, most preferably 2 hours to obtain uncoated drop pills.
  • 17. The preparation method according to the 16th paragraph, wherein in Step (4), a gradient-rising temperature drying method is used as follows: fluidizing at −20˜30° C., drying at 15˜35° C. for 10˜120 min, drying at 35˜55° C. for 10˜60 min, drying at 55˜100° C. for 0˜60 min; preferably, the gradient-rising temperature drying method is performed as follows: fluidizing at 0˜20° C., drying at 25° C. for 60 min, drying at 45° C. for 30 min, drying at 55° C. for 0˜30 min.
  • 18. The preparation method according to any one of the 1st˜17th paragraphs, wherein the method additionally comprises a coating step as Step (5): coating the uncoated drop pills obtained from Step (4) in a state of fluidization; the concentration of the coating liquid is at 15˜25 wt %, preferably 18˜20 wt %; the coating material is selected from shellac, CAP (cellulose acetate phthalate), methyl acrylate, methyl methacrylate or Opadry; the ratio of the coating material to the uncoated drop pill is 1:50˜1:25 by weight.
  • 19. The preparation method according to any one of the 1st˜18th paragraphs, wherein the method additionally comprises a pre-mixing step before Step (1): adding the medicine powder or extract with water, stirring for 10 min or longer at 30˜80° C. to obtain a pre-mixed medicine material.
  • As the second aspect of this invention, the present invention includes the following technical solutions:
  • 20. A TCM formulation of micro drop pill, wherein in the micro drop pill, the ratio of the medicine to the drop pill matrix is 1:5˜5:1 by weight, a particle size of the micro drop pill is 0.2 mm˜4 mm, the micro drop pill is prepared by any one method of the 1st˜19th paragraphs, and the micro drop pill has no residual coolant.
  • 21. The TCM formulation of micro drop pill according to the 20th paragraph, characterized in that the particle size is 0.2 mm˜2 mm.
  • 22. The TCM formulation of micro drop pill according to the 21st paragraph, characterized in that the particle size is 1 mm˜2 mm.
  • 23. A Compound Salvia Militiorrhiza micro drop pill (CSMDP), wherein the micro drop pill is prepared by the API of Compound Salvia Militiorrhiza and the drop pill matrix in a ratio of 1:5˜5:1 by weight, the particle size of the Compound Salvia Militiorrhiza micro drop pill is 0.2 mm˜4 mm, the API of Compound Salvia Militiorrhiza is prepared by the following crude drugs by weight parts: Salvia Militiorrhiza 75.0˜90.0 parts, Panax Notoginseng 10.0˜25.0 parts and borneol 0.1˜4.0 parts, and the micro drop pill is prepared by any one method of the 1st˜19th paragraphs, and the micro drop pill has no residual coolant.
  • 24. The CSMDP according to the 23rd paragraph, wherein the micro drop pill is prepared by the API of Compound Salvia Militiorrhiza and the drop pill matrix in a ratio of 1:3˜3:1 by weight.
  • 25. The CSMDP according to the 24th paragraph, wherein the micro drop pill is prepared by the API of Compound Salvia Militiorrhiza and the drop pill matrix in a ratio of 1:(1˜3) by weight.
  • 26. The CSMDP according to any one of the 23rd˜25th paragraphs, characterized in that the particle size of the micro drop pill is 0.2 mm˜2 mm.
  • 27. The CSMDP according to the 26th paragraph, characterized in that the particle size of the micro drop pill is 1 mm˜2 mm.
  • 28. The CSMDP according to any one of the 23rd˜27th paragraphs, wherein the API of Compound Salvia Militiorrhiza is prepared by the following crude drugs by weight parts: Salvia Militiorrhiza 80.0˜86.0 parts, Panax Notoginseng 15.0˜18.0 parts and borneol 0.2˜2.0 parts.
  • 29. The CSMDP according to any one of the 23rd˜28th paragraphs, wherein the API of Compound Salvia Militiorrhiza is prepared by the following crude drugs by weight parts: Salvia Militiorrhiza 82.0˜84.0 parts, Panax Notoginseng 16.0˜17.0 parts and borneol 0.4˜1.2 parts.
  • 30. A Qishenyiqi micro drop pill (QMDP), characterized in that the micro drop pill is prepared by the API of Qishenyiqi and the drop pill matrix in a ratio of 1:5˜5:1 by weight, the particle size of the Qishenyiqi micro drop pill is 0.2 mm˜4 mm, the API is prepared by the following crude drugs by weight parts: Astragalus membranaceus 100˜200 parts, Salvia Militiorrhiza 50˜100 parts, Panax Notoginseng 10˜20 parts and volatile oil from Lignum Dalbergiae Odoriferae 0.5˜2 parts, the micro drop pill is prepared by any one method of the 1st˜19th paragraphs, and the micro drop pill has no residual coolant.
  • 31. The QMDP according to the 30th paragraph, wherein the QMDP is prepared by the API of Qishenyiqi and the drop pill matrix in a ratio of 1:3˜3:1 by weight.
  • 32. The QMDP according to the 31st paragraph, wherein the QMDP is prepared by the API of Qishenyiqi and the drop pill matrix in a ratio of 1:(1˜3) by weight.
  • 33. The QMDP according to any one of the 30th˜32nd paragraphs, wherein the particle size of the micro drop pill is 0.2 mm˜2 mm.
  • 34. The QMDP according to the 33rd paragraph, wherein the particle size of the micro drop pill is 1 mm˜2 mm.
  • 35. The QMDP according to any one of the 30th˜34th paragraphs, wherein the API of Qishenyiqi is prepared by the following crude drugs by weight parts: Astragalus membranaceus 150˜180 parts, Salvia Militiorrhiza 75˜85 parts, Panax Notoginseng 13˜18 parts and volatile oil from Lignum Dalbergiae Odoriferae 0.5˜1 parts.
  • 36. The QMDP according to any one of the 30th˜35th paragraphs, wherein the API of Qishenyiqi is prepared by the following crude drugs by weight parts: Astragalus membranaceus 150 parts, Salvia Militiorrhiza 75 parts, Panax Notoginseng 15 parts and volatile oil from Lignum Dalbergiae Odoriferae 1 part.
    • DETAILED DESCRIPTION OF THE INVENTION
  • In an embodiment of this invention, the preparation method for preparing the micro drop pill comprises the following steps:
  • (1) Material melting step: heat melting the medicine and the drop pill matrix at 40° C.˜−120° C., homogenizing for 0.5˜4 hours to obtain a homogenized molten medicine liquid, the ratio of the medicine to the drop pill matrix is 1:5˜5:1 by weight;
  • (2) Dropping step: delivering the molten medicine liquid under pressure to a dripper, and acquiring medicine drops at a vibration frequency for dropping of 2˜2000 Hz under a dropping pressure of 0.5˜4.0 Bar, the temperature of the dripper of 40° C.˜−200° C. and the viscosity of the molten medicine liquid of 300˜1500 cp; and,
  • (3) Condensation step: cooling the medicine drops with a cooling gas for forming by solidifying, obtaining the micro drop pills having a particle size of 0.2 mm˜4 mm, the temperature of the cooling gas is 0° C. or lower.
  • Wherein, in Step (1), the drop pill matrix includes one or more selected from the group consisting of PEGs, sorbitol, xylitol, lactitol, maltose, starch, methylcellulose, sodium carboxymethyl cellulose, hydroxypropyl methylcellulose (HPMC), arabic gum, alginic acid, dextrin, cyclodextrin, agar and lactose, preferably solid PEGs, such as PEG-1000, PEG-2000, PEG-3000, PEG-4000, PEG-5000, PEG-6000, PEG-7000 and PEG-8000, more preferably one or more selected from the group consisting of PEG-1000, PEG-2000, PEG-3000, PEG-4000, PEG-6000, PEG-8000, most preferably PEG-6000, PEG-4000 or the combination of PEG-4000 and PEG-6000.
  • In Step (1), the temperature for heat melting preferably is at 60˜100° C., more preferably at 65˜90° C., further preferably 75˜85° C.
  • In Step (1), the homogenizing time preferably is 1˜3 hours, further preferably 2 hours.
  • In Step (1), the ratio of the medicine to the drop pill matrix is 1:3˜3:1 by weight, preferably 1:(1˜3) by weight.
  • In Step (2), the temperature of the dripper is preferably at 60˜120° C., preferably at 60˜100° C.; the vibration frequency for dropping is preferably at 20˜300 Hz, more preferably 50˜300 Hz, more preferably 20˜200 Hz, more preferably 20˜150 Hz, most preferably 50˜150 Hz. The vibration mode includes magnetic/electronic vibration or pneumatic vibration. Wherein, in the pneumatic vibration mode, the vibration frequency and the vibration amplitude are larger. If the material viscosity is more than 800 cp, the electronic vibration is incapable of effectively cutting material, resulting in the blockage of the dripper; if this happens, the pneumatic vibration mode can be used. In the present invention, the electronic vibration is preferably employed, the viscosity of the molten medicine liquid preferably is 500˜1000 cp, more preferably 700˜1000 cp.
  • During the dropping process, a vibration waveform is used as a PAT (Process Analyzing Technology) index to measure the distribution of the particle size and to monitor the state of fluidization of the drop pills in the real-time manner by using a stroboscopic device.
  • In Step (3), the condensation by a cooling gas means that the drops are cooled by using a low-temperature condensate trap to form by solidifying. The temperature of the cooling gas is at 0° C.˜−150° C., preferably −10° C.˜−140° C., further preferably −40° C.˜−140° C., further preferably −60° C.˜−140° C., most preferably −80° C.˜−120° C.; the cooling gas is air, nitrogen or inert gas; the particle size of the micro drop pill is 1.0 mm˜2.0 mm, preferably 0.5 mm˜2 mm.
  • In one preferred embodiment of this invention, the preparation method for preparing the micro drop pill comprises the following steps:
  • (1) Material melting step: heat melting the medicine and the drop pill matrix at 60° C.˜−100° C., homogenizing for 1˜3 hours to obtain a homogenized molten medicine liquid, the ratio of the medicine to the drop pill matrix is 1:3˜3:1 by weight;
  • (2) Dropping step: delivering the molten medicine liquid under pressure to a dripper, and acquiring medicine drops at a vibration frequency for dropping of 20˜200 Hz under a dropping pressure of 0.5˜4.0 Bar, the temperature of the dripper of 60° C.˜−120° C. and the viscosity of the molten medicine liquid of 700˜1000 cp; and,
  • (3) Condensation step: cooling the medicine drops with a cooling gas for forming by solidifying, obtaining the micro drop pills having a particle size of 0.5 mm˜2 mm, the temperature of the cooling gas is 0° C.˜−150° C.
  • In another preferred embodiment of this invention, the preparation method for preparing the micro drop pill comprises the following steps:
  • (1) Material melting step: charging the medicine and the drop pill matrix into a homogenizer, mixing homogenously at 1000˜5000 rpm for 1˜200 min, then melting homogenously at 3000˜10000 rpm for 1˜100 min; during the melting process, the temperature is kept at 60˜100° C. to obtain the molten medicine liquid; the ratio of the medicine to the drop pill matrix is 1:5˜5:1 by weight;
  • (2) Dropping step: delivering the molten medicine liquid to a dripper, and acquiring medicine drops by means of vibration dropping at a vibration frequency for dropping of 20˜300 Hz under a dropping pressure of 0.5˜4.0 Bar and the temperature of the dripper of 40° C.−200° C.; the dropping rate is matched with the melting rate in Step (1); and,
  • (3) Condensation step: cooling the medicine drops with a cooling gas rapidly to solidify, and obtaining solid drop pills having a particle size of 0.2 mm˜-4.0 mm; the temperature of the cooling gas is 0° C.˜−150° C.
  • Wherein, in Step (1), the ratio of the medicine to the drop pill matrix is 1:3˜3:1 by weight, mixing homogeneously 3000˜5000 rpm for 10˜60 min and melting homogeneously at 4000˜9000 rpm for 5˜30 min, during the melting process, the temperature is kept at 70˜90° C.; most preferably, the ratio of the medicine to the drop pill matrix is 1:(1˜3) by weight, mixing homogeneously 3000˜4000 rpm for 10˜30 min and melting homogeneously at 4000˜6000 rpm for 6˜30 min, during the melting process, the temperature is kept at 75˜85° C.
  • In Step (2), preferably, the temperature of the dripper is at 70˜100° C., the vibration frequency for dropping is at 90˜200 Hz, the dropping pressure is at 1.0˜3.0 Bar; most preferably, the vibration frequency is at 137 Hz, the acceleration speed is at 4G, the dropping pressure is at 1.8 Bar and temperature of the dripper is at 75˜85° C.; Preferably, the dropping rate is 10˜40 Kg/h, preferably 12˜30 Kg/h, further preferably 15˜25 Kg/h. Further, the method can additionally comprise a drying step as Step (4): drying the low-temperature drop pills from Step (3) on a fluidized-bed at 40˜150° C., preferably at 40˜60° C. for 1˜4 hours, preferably 1˜3 hours, most preferably 2 hours to obtain the uncoated drop pills.
  • In Step (4), a gradient-rising temperature drying method is used as follows: fluidizing at −20˜30° C., drying at 15˜35° C. for 10˜120 min, drying at 35˜55° C. for 10˜60 min, drying at 55˜100° C. for 0˜60 min; preferably, the gradient-rising temperature drying method is performed as follows: fluidizing at 0˜20° C., drying at 25° C. for 60 min, drying at 45° C. for 30 min, drying at 55° C. for 0˜30 min.
  • In Step (4), by screening from a large number of drying methods, the inventors found that: in Step (3), the uncoated drop pill is dried by one of the following drying methods: airing under low-humidity, drying by coating pot, drying by vacuum drying oven, drying by hot air circulation drying oven, drying by track type microwave dryer, drying by fluidized drying coater. In terms of yield and productivity, drying by coating pot, drying by track type microwave dryer, drying by fluidized drying coater are preferred. In terms of industrialization, drying by fluidized-bed is preferred, and drying by fluidized drying coater is more preferred. Advantages and disadvantages of various drying methods are shown in Table 1.
  • TABLE 1
    Nos. Drying mode Advantages Disadvantages
    1 Airing under High yield. The yield is usually (1) Stringent requirement for airing environment,
    low-humidity about 95% without considering the demanding clean air-circulated workshops with a
    effect of dropping factor. relative humidity of less than 30%, a temperature
    of higher than 20° C. and a good air circulation;
    (2) Prolonged drying period, at least 48 hours
    required when a layer thickness of the drop pills
    is up to about 2 cm;
    (3) Large-area workshop is occupied;
    (4) Regularly turning the drop pills is necessary;
    (5) Exposing for a long time, the drop pill product
    is prone to being polluted.
    2 Drying by (1) High yield. The yield is usually (1) Demanding the inlet air having a low humidity,
    coating pot about 95% without considering the generally no more than 5 g/kg;
    effect of dropping factor; (2) Low drying efficiency, at least 6 h/batch;
    (2) Drying and coating can be achieved (3) Custom-made device;
    in one machine. (4) Easily resulting in product rejection due to
    the adhesion of drop pills.
    3 Drying by vacuum None (1) Low drying efficiency, demanding low-temperature
    drying oven vacuum drying for a long time, at least 30 h/batch;
    (2) Low-productivity device, the productivity of oven
    per square meter is difficult to exceed 0.2 kg/h;
    (3) Easily resulting in adhesion and deformation of
    drop pills, which is not round in appearance.
    4 Drying by hot None (1) Low drying efficiency, demanding low-temperature
    air circulation drying for a long time, at least 40 h/batch;
    drying oven (2) Low-productivity device, the productivity of oven
    per square meter is difficult to exceed 0.1 kg/h;
    (3) Easily resulting in adhesion and deformation of
    drop pills, which is not round in appearance;
    (4) Relative humidity in the drying workshop should
    be less than 30%.
    5 Drying by track type High yield, reaching 20 Kg/h (1) Difficult to control the drying process, easily
    microwave dryer resulting in adhesion and deformation of drop pills,
    which is not round in appearance, or product rejection
    due to charring by drying;
    (2) Relative humidity in the drying workshop is less
    than 30%;
    (3) Unable to remove residual microwave in product.
    6 Drying by fluidized (1) High yield, reaching 30 kg/h; Necessary to control inlet air humidity, generally no
    drying coater (2) Dying and coating in one machine; more than 7.5 g/kg.
    (3) Round drop pill in appearance;
    (4) High yield, the yield is usually
    98% or higher without considering the
    effect of dropping factor;
    (5) Easy to control the drying process,
    real-time displaying the water-content
    in the drop pills.
  • Further, the preparation method for the micro drop pill can additionally comprise a coating step as Step (5): coating the uncoated drop pills obtained from Step (4) in a state of fluidization; the concentration of the coating liquid is at 15˜25 wt %, preferably 18˜20 wt %; the coating material is selected from shellac, CAP (cellulose acetate phthalate), methyl acrylate, methyl methacrylate or Opadry; the ratio of the coating material to the uncoated drop pills is 1:50˜1:25 by weight.
  • In the present invention, in order to better implement the preparation method for the micro drop pill, preferably, the method can additionally comprise a pre-mixing step before Step (1): adding the medicine powder or extract with water, stirring for 10 min or longer at 30˜80° C. to obtain a pre-mixed medicine material, ensuring the homogenization of water content. This step can remedy the defects brought about by feeding dried powder material.
  • In the present invention, the micro drop pills prepared by the method can be either packaged directly, or prepared into capsule after loading into a capsule shell. In the preparation of capsules, the weighing step for capsules one-by-one may be additionally employed. Before packaging, high-speed weighing for the loaded capsules one-by-one is employed so as to eliminate possibly unqualified capsules.
  • In the present invention, the features of the method are as follows: it is the first time to combine the techniques of vibration dropping and gas cooling with the fluidized drying & coating method creatively and apply to the preparations of drop pills and drop pill capsules. Hence, both producing rate and forming quality of the drop pill are increased.
  • Further the production process is simplified. The advantages of the present invention are presented as follows:
  • 1. Using a Method of Vibration Dropping Plus Gas Cooling Instead of the Traditional Drop Pill Preparation Method (Gravity Dropping/Pressurized Dropping and Coolant Cooling)
  • Utilization of gas cooling well meets the requirements of high-speed dropping, preparing a micro drop pill (with a particle size of 2.5 mm or smaller) and increasing drug-loading capacity. As a result, the drug-loading capacity of the drop pill has been increased by folds while the amount of the drop pill matrix and the dosage are reduced dramatically. Moreover, the productivity of the drop pills has been enhanced greatly from the traditional rate of 1˜2 pills/s to 1000˜1250 pills/s, and the range of the particle size is expanded from 2 mm˜4 mm to 0.2 mm˜4 mm. It is possible to produce the micro drop pills that can better meet the requirements for capsule loading. By adjusting the vibration parameters and fluidized drug loading coating, the drug-loading capacity can be increased from about 25 wt % of the traditional drop pills to 50 wt % and higher, and the amount of the drop pill matrix is also reduced by leaps and bounds.
  • 2. Instead of the traditional coolant of liquid paraffin and silicone oil etc, the low-temperature air, nitrogen or inert gas are used to cool the drop pills, avoiding the follow-up steps of eliminating residual solvent (e.g. subsequent step of removing oil). Hence, the operation process is simplified and totally no residual organic solvent. The preparation cost is also reduced.
  • 3. By adding fluidized drying & coating process, not only can solve the problems during the storage of the drop pills prepared by air drying method such as possible adhesion of the drop pills from each other, precipitation of components and reduced volatile oil components, but also the drying time can be reduced from 4˜24 hours to only 2 hours. By using fluidized coating, the molten medicine liquid was injected to make drug-loading coating, and the drug-loading capacity can be further increased. Also, this technique of injection can be used for coating the drop pills so as to realize the purposes of different techniques (e.g. sustained release coating, film coating and sugar coating etc). Because the fluidization is a mild process, it ensures the water content in the drop pill reaches a stable value, and the uniformity in drug-loading and coating in the drop pills are also improved. Unlike the drop pills prepared by the traditional methods, the fluidization can prevent the drop pills from being cleft and white-dotted, and at the same time, the yield is increased.
  • Comparison of the physico-chemical parameters between the micro drop pills of the present invention and the current drop pills are summarized in Table 2.
  • TABLE 2
    Pill weight & Drug-loading Roundness &
    volume capacity Appearance Preparation efficiency Release rate particle size
    Micro drop Smaller pill Drug-loading gas cooling instead of By using super high-speed Mixing the medicine with the Excellent
    pills of the weight, about 30 wt % traditional coolant, vibration dropping device and drop pill matrix by roundness, the
    present 4 mg, so the (calculated ensuring pressurized dropping mode, homogenizer, so the API of drop pill with
    invention filling based on condensation forming ensuring a stable delivery of the medicine fully dispersed, a particle size
    amount is dried extract) effect, overcoming the material, increasing thus helping drug absorption. of
    more the drawbacks of dropping rate, greatly Additionally, reduced pill 0.2 mm~4 mm
    accurate residual coolant improving the preparation weight makes the filling can be
    when being efficiency. amount more accurate when prepared.
    filled into being filled into capsule, drug
    capsule shell release rate is also
    accelerated, and thus a
    clinical efficacy is improved.
    Commercially Larger pill Drug-loading Residual coolant on Slower dropping rate than that Better
    available drop weight, 18~20 wt % the surface of the of the vibration dropping, and roundness, the
    pills 25 mg~27 mg (calculated drop pills complicated process of drop pill with a
    based on eliminating the coolants on particle size of
    dried extract) the surface of the drop pills, 1 mm~2 mm
    time-consuming process. cannot be
    prepared.
    • EXAMPLES
  • The following examples are offered only for the purposes of detailed explanation of the present invention and are not intended to limit the scope of the invention in any way.
    • Example 1 Compound Salvia Militiorrhiza Micro Drop Pill (CSMDP)
  • Compound Salvia Militiorrhiza Drop Pill is a TCM developed by Tianjin Tasly Pharmaceutical Co., Ltd, which is proven to have effects of activating blood by removing stasis and stopping pain by regulating Qi, used for treating chest distress and angina pectoris. The main ingredients of Compound Salvia Militiorrhiza Drop Pill include Salvia Militiorrhiza, Panax Notoginseng and borneol. Its pharmacological effects include increasing coronary blood flow, protecting ischemia myocardium by strengthening hypoxia tolerance, preventing thrombosis by anti-platelet aggregation and improving microcirculation etc.
  • The current Compound Salvia Militiorrhiza Drop Pill was prepared by the following method: extracting Salvia Militiorrhiza and Panax Notoginseng with water to give an extraction liquid, which was followed by concentration to get the extract; mixing the extract with the drop pill matrix, delivering to a dropping machine, into which borneol was added and well mixed to get a material; melting and dropping the material, and cooling the medicine drops by using liquid paraffin as a coolant to obtain Compound Salvia Militiorrhiza Drop Pill. Although the preparation of Compound Salvia Militiorrhiza Drop Pill was known as a very mature technique by the person skilled in the art, there were still a lot of problems faced during the preparation process, e.g. large amount of the matrix and a small unit drug-loading capacity.
  • In the present invention, the CSMDP is prepared by the API of Compound Salvia Militiorrhiza and the drop pill matrix in a ratio of 1:5˜5:1 by weight; preferably 1:3˜3:1 by weight; most preferably 1:(1˜3) by weight.
  • The API of Compound Salvia Militiorrhiza is prepared by the following crude drugs by weight parts:
  • Salvia Militiorrhiza 75.0˜90.0 parts
  • Panax Notoginseng 10.0˜25.0 parts
  • borneol 0.1˜4.0 parts.
  • Preferably, the API of Compound Salvia Militiorrhiza is prepared by the following crude drugs by weight parts:
  • Salvia Militiorrhiza 80.0˜86.0 parts
  • Panax Notoginseng 15.0˜18.0 parts borneol 0.2˜2.0 parts.
  • Most preferably, the API of Compound Salvia Militiorrhiza is prepared by the following crude drugs by weight parts:
  • Salvia Militiorrhiza 82.0˜84.0 parts
  • Panax Notoginseng 16.0˜17.0 parts
  • borneol 0.4˜1.2 parts.
  • In the present invention, the API of Compound Salvia Militiorrhiza is believed to be the active pharmaceutical ingredient of CSDP, which is prepared by extracting Salvia Militiorrhiza and Panax Notoginseng to give the extract and mixing borneol to obtain the product. The preparation of the API belongs to the prior art, and the API can be prepared by the conventional methods with the crude drugs in the ratios of the present invention, or by the commercially available Salvia Militiorrhiza extract, Panax Notoginseng extract and borneol. In order to better achieve the invention, the API of Compound Salvia Militiorrhiza is preferably prepared by the following method:
  • (1) Decocting Salvia Militiorrhiza and Panax Notoginseng with water under an alkaline condition to give a decoction, filtering the decoction, concentrating and precipitating the filtrate with ethanol to get a supernatant, filtering the supernatant, recovering ethanol and drying to give Salvia Militiorrhiza and Panax Notoginseng extract;
  • (2) Adding the extract of the above step with borneol and mixing to give the API.
  • Preferably, in Step (1), under an alkaline condition, Salvia Militiorrhiza and Panax Notoginseng are decocted for 1˜3 times, 1˜3 hours each time and the decoction is filtered to get a filtrate (Filtrate I) for later use; dregs of the decoction is further decocted with water for 1˜3 times, 1˜3 hours each time, the decoction is filtered to get a filtrate (Filtrate II) for later use; Filtrate I and Filtrate II are combined and concentrated to give a concentrated liquid, which is precipitated with ethanol and allows to stand still to get a supernatant; the supernatant is filtered, ethanol therein is recovered, and further concentrated to give the Salvia Militiorrhiza and Panax Notoginseng extract.
  • The alkaline condition includes, but not limited to, one or more kinds alkali selected from the group consisting of sodium bicarbonate, sodium carbonate, disodium hydrogen phosphate, sodium dihydrogen phosphate, sodium hydroxide, potassium hydroxide and magnesium hydroxide; a pH value of 7.5˜9.0 is preferred, ensuring sodium danshensu (sodium DL-beta-(3,4-dihydroxyphenyelactate) can be extracted totally.
  • Preferably, 50˜100% (v/v) (most preferably 95% (v/v)) ethanol solution is added to perform ethanol-precipitation, the final content of ethanol preferably is 60˜75% (v/v).
  • The preparation method for preparing the CSMDP comprises the following steps:
  • (1) Material melting step: charging the API of Compound Salvia Militiorrhiza and the drop pill matrix in a ratio of 1:5˜5:1 by weight into a homogenizer, mixing homogenously at 1000˜5000 rpm for 1˜200 min, then melting homogenously at 3000˜10000 rpm for 1˜100 min; during the melting process, the temperature is kept at 60˜100° C. to obtain a molten medicine liquid;
  • (2) Dropping step: delivering the molten medicine liquid to a dripper, and acquiring medicine drops by means of vibration dropping at a vibration frequency of 50˜300 Hz under a dropping pressure of 0.5˜4.0 Bar, the temperature of the dripper is at 70° C.˜−200° C.; the dropping rate is matched with the melting rate in Step (1); and,
  • (3) Condensation step: cooling the medicine drops with a cooling gas rapidly to solidify, and obtaining uncoated drop pills having a particle size of 0.2 mm˜-4 mm; the temperature of the cooling gas is 0° C.˜−150° C.
  • After Step (2) and Step (3), the pill weight is decreased from 23.5˜27.5 mg of the traditional drop pill to 3˜4 mg, which can be loaded into capsules; in addition, the problem of residual coolant such as liquid paraffin in the current drop pill product can be solved by using gas cooling.
  • In order to better prove the merits of the micro drop pill in the present invention, the trial was presented as follows:
    • Trial Example 1 Comparative Study on Effects of Two Kinds of CSDPs on Acute Myocardial Infarction in Rats 1. Animals
  • SD male rats, weighing 340˜360 g, were purchased from Beijing Weitonglihua Experimental Animal Co., Ltd, and certification No.: SCXK (Jing) 2007-0001.
    • 2. Drugs, Reagents and Apparatus
  • CSMDP of the present invention was prepared by the method of Preparative Example 1 of CSMDP.
  • CSDP, used as a comparative drug, was commercially available in China, prepared by Tianjin Tasly Pharmaceutical Co., Ltd.
  • Chloral hydrate and triphenyl tetrazolium chloride (TTC) were used for anesthesia.
  • Apparatus: MedLab-U/8c bio-signals collecting-processing system, purchased from Nanjin Meiyi Inc.
    • 3. Experimental Methods
  • Grouping: the rats were randomly divided into groups according to their body weight: S group (Sham operation group), M group (Model group), Y group (Positive control group, metoprolol tartrate, Lot No. 1201039), F group (CSMDP of the present invention) and G group (CSDP available in China, Lot No. 2011L16); 10 rats in each group.
  • Modeling and Administrating Method:
  • After grouping, the animals were administrated intragastrically for 7 days, which was shown in Table 3. On the 8th day, the rats were anesthetized intraperitoneally with 10% chloral hydrate (3 ml/kg) and fixed on a small wood plate in a supine position. Pins were inserted under the skin of the right forelimb and both hind limbs, and then the rats were connected with the MedLab-U/8c bio-signals collecting-processing system to record ECG of the rats. Hair on the front wall of the left chest was clipped. Oral tracheal cannula was performed and the animal respirator was connected at a respiratory frequency of 80 breaths/min, tidal volume 3 ml/100 g and I:E=1:1. Chest on the left front chest lateral side was incised to cut the 3′ rib and the pericardium was carefully lifted with forceps to tear apart. The left main trunk of coronary vein pass between the lower edge of the left atrial appendage and pulmonary artery cone was observed in most of the rats, accompanied with left anterior decending branch (LAD). Medical suture (4-0) was used to transfix LAD and a small amount of myocardial tissue at a distance of about 1˜2 mm from the lower edge of the left atrial appendage and inside interventricular sulcus in the vicinity of the left main trunk of coronary vein. The rats with an elevated J point by 0.1 mV in ECG and pale LVAW (left ventricular anterior wall) indicated a successful modeling. Chest was closed layer by layer. The tracheal tube was removed until the voluntary respiration was recovered in the rats. ECG was recorded continuously for 4 hours. Rats were anesthetized, their heart were cut out, sliced and dyed to calculate myocardial infarction rate (MIR). The serum was collected for later use.

  • MIR (%)=wet weight of the infarction region/wet weight of the whole heart×100%
  • TABLE 3
    Grouping and administration
    Pre-
    Dosage administration
    Groups (mg/kg) Dose time
    S group(Sham operation 110 1 ml/100 g 7 d
    group)
    M group(Model group) 223 1 ml/100 g 7 d
    Y group(Positive control 4.5 1 ml/100 g 7 d
    group, metoprolol tartrate)
    G group(CSDP available in 115 1 ml/100 g 7 d
    China)
    F group(CSMDP of the 84 1 ml/100 g 7 d
    present invention)
    • 4. Results 4.1 Effect on MIR
  • The results were presented in Table 4. As shown in Table 4, 7 days after pre-administration, MIR in M group (Model group) was significantly higher than the one in S group (Sham operation group), suggesting the successful modeling. MIRs in G group and F group were respectively 3.38% and 3.32%, significantly lower than the one in M group (5.07%), having a significant difference (p<0.01). It was indicated that both samples had a certain effect against the acute myocardial infarction. However, there was no significantly statistical difference (p>0.05) between G group and F group.
  • TABLE 4
    Effect of CSDP in each group on MIR
    Average wet Average wet
    weight of weight of
    the whole the infarction
    Groups N heart (g) region (g) MIR (%)
    S group 8 0.8254 ± 0.0294 0.0000 ± 0.0000 0.00 ± 0.00 
    M group 10 0.8207 ± 0.0447 0.0414 ± 0.0051 5.07 ± 0.75 
    Y group 9 0.8783 ± 0.0571 0.0233 ± 0.0038 2.65 ± 0.33* 
    G group 10 0.8493 ± 0.0641 0.0288 ± 0.0052 3.38 ± 0.49*#
    F group 10 0.8061 ± 0.0668 0.0268 ± 0.0054 3.32 ± 0.59*#
    Noted:
    compared with M group (Model group), *p < 0.01;
    compared with Y group (Positive control group), #p < 0.01.

    4.2 Effect on the Heart Rate in Rats with Myocardial Infarction
  • As shown in Table 5, the descending order of the heart rate was F group, G group, M group, Y group and S group within the observation period and 0˜1 hour after ligation. 1 hour later, the heart rate in each group was decreased. Within the observation period, the variation of heart rate in Y group and S group was relatively stable. There was no significant difference among these groups in heart rate of the rats.
  • TABLE 5
    Effect of the CSDP sample in each group on the heart rate (beat/min)
    Groups N 0 s 5 s 10 s 5 min 10 min 30 min 1 h 2 h 3 h 4 h
    S 8 390 ± 50 390 ± 52 400 ± 51 407 ± 43 401 ± 57 386 ± 69 394 ± 58 417 ± 44 364 ± 42 358 ± 36
    group
    M 10 416 ± 83 447 ± 72 436 ± 67 444 ± 43 423 ± 39 423 ± 32 399 ± 31 361 ± 45 363 ± 46 336 ± 59
    group
    Y 9 377 ± 48 423 ± 39 419 ± 41 424 ± 29 431 ± 17 413 ± 34 421 ± 47 416 ± 33 380 ± 66 395 ± 52
    group
    G 10 431 ± 43 452 ± 21 444 ± 24 445 ± 29 424 ± 27 422 ± 25 397 ± 25 392 ± 40 347 ± 39 331 ± 38
    group
    F 10 449 ± 28 498 ± 7 468 ± 34 474 ± 35 466 ± 34 426 ± 40 412 ± 40 388 ± 51 377 ± 60 365 ± 56
    group
    • 5. Conclusions
  • Under the dosage set in the trial, the medicines in each group were proven to have a certain effect against myocardial infarction in the rats with a coronary artery ligature; especially the CSMDP of the present invention at a dosage of 84 mg/kg had a MIR of 3.38±0.49%, having a similar efficacy of MIR (3.32±0.59%) of the CSDP product commercially available in China at a dosage of 115 mg/kg. Obviously, the CSMDP at a dosage of 84 mg/kg reached the same effect with the CSDP product commercially available in China at a dosage of 115 mg/kg. The CSMDP had a better efficacy than the current CSDP, having the merits such as high bioavailability, reduced administration dosage and good compliance to the patients, etc.
    • CSMDP Preparative Example 1
  • The following materials were prepared: 75 g of Salvia Militiorrhiza and Panax Notoginseng extract, 7.5 g of borneol and 165 g of PEG-6000.
  • (1) Pre-mixing step: the API of Compound Salvia Militiorrhiza was added with water to pre-mix, stirred in a heat-insulated tank at 40±10° C. for 60 min or longer to make the water content of the API of Compound Salvia Militiorrhiza at 13.0 wt % to give a pre-mixed material of the API of Compound Salvia Militiorrhiza for later use;
  • (2) Material melting step: the PEG-6000 was firstly added into a melting tank, pre-molten by heating to 90° C., into which the pre-mixed material of the API of Compound Salvia Militiorrhiza was added and the resultant material was mixed by a low-speed homogenization (3200 rpm); after mixing, the homogenization rate was increased to 5000 rpm to melt the material for 6 min; during melting process, the temperature of the material was kept at 80±5° C. to give a molten medicine liquid;
  • (3) Dropping step: the aforesaid molten medicine liquid was delivered to a dripper, the vibration frequency of the dripper was adjusted to 137 Hz and the temperature of the dripper was adjusted to 80° C.; the medicine liquid was flowed under pressure (1.8 Bar) into the dripper, from the bottom of which the medicine liquid was dropped down by means of vibration; the dropping rate was matched with the melting rate in Step (1);
  • (4) Condensation step: the medicine drops were cooled in a cooling duct with a low-temperature inert gas at −115±5° C. to cool the liquid drops to form solid drop pills;
  • (5) Drying step: the resultant drop pills were dried in a fluidized state; until the drop pills reached a better fluidized state in the bed of the fluidized bed, the temperature was increased to 25° C. to dry for 60 min, further increased to 45° C. to dry for 30 min, continuously increased to 55° C. to dry for 30 min, and decreased 30° C. or lower to discharge the drop pills. The water content of the drop pills was controlled in the range of 3.0˜7.0 wt % to give uncoated drop pills as the intermediate product;
  • (6) Coating step: the amount of coating powder was calculated based on the coating feed capacity and formulation; Opadry, which has 4 wt % of the weight of the uncoated drop pills, was used to prepare a 18 wt % coating solution and stirred for 45 min; the inlet air temperature was initially set to 25° C.; after the qualified uncoated drop pills were loaded into the fluidized bed, the inlet air temperature was increased to 48° C.; until the temperature of the materials was up to 38° C., the coating was started; the temperature of the material was kept at 35˜45° C. during the coating and decreased 30° C. or lower after coating; the drop pills were discharged, screened to give coated drop pills as the intermediate product, the coating weigh of the coated drop pills was controlled in a range of 3.3±0.7 wt % and the water content was controlled in a range of 3.0˜7.0 wt %;
  • (7) Loading into capsule and packaging step: the resultant micro drop pills with a particle size of 1.0 mm˜2.0 mm were loaded into capsules; 100% of the capsules were on-line checkweighed with a capsule checkweigher, packaged to give the final product.
  • Wherein, during the dropping process, the formation of the drop pills was measured visually by using a stroboscopic illumination to perform a real-time monitoring and adjustment. In order to improve the uniformity and roundness of the drop pills, the steps of screening and regulating the drop pills could be added.
  • Wherein, the API of Compound Salvia Militiorrhiza was prepared by the following method:
  • (1) 83.0 kg of Salvia Militiorrhiza and 16.0 kg of Panax Notoginseng were decocted with water under an alkaline condition to give a decoction; the decoction was filtered, concentrated and precipitated with ethanol to give a supernatant; the supernatant was filtered, recovered ethanol and dried to give the Salvia Militiorrhiza and Panax Notoginseng extract; and,
  • (2) 0.8 kg of borneol was added to the aforesaid Salvia Militiorrhiza and Panax Notoginseng extract and well mixed to obtain the API.
  • Wherein, in Step (1), under an alkaline condition (pH 8.0), Salvia Militiorrhiza and Panax Notoginseng were decocted for 2 times, 2 hours each time and filtered to give Filtrate I for later use; dregs of the decoction was further decocted with water for 2 times, 2 hours each time, filtered to give Filtrate II for later use; Filtrate I and Filtrate II were combined and concentrated to give a concentrated liquid, which was added with ethanol to make the final content of ethanol as 70% (v/v) and allowed to stand still to give a supernatant; the supernatant was taken, filtered, ethanol therein was recovered, concentrated and dried to give the Salvia Militiorrhiza and Panax Notoginseng extract.
  • Besides, borneol was commercially available.
    • CSMDP Preparative Example 2
  • Except that the Salvia Militiorrhiza and Panax Notoginseng extract was prepared by the following crude drugs by weight parts: Salvia Militiorrhiza 75 parts, Panax Notoginseng 10 parts, borneol 0.1 parts, and the ratio of the API of Compound Salvia Militiorrhiza to PEG-6000 was 1:5 by weight, the CSMDP was prepared by the same method as CSMDP PREPARATIVE EXAMPLE 1.
    • CSMDP Preparative Example 3
  • Except that the Salvia Militiorrhiza and Panax Notoginseng extract was prepared by the following crude drugs by weight parts: Salvia Militiorrhiza 90 parts, Panax Notoginseng 25 parts, borneol 4 parts, and the ratio of the API of Compound Salvia Militiorrhiza to PEG-6000 was 5:1 by weight, the CSMDP was prepared by the same method as CSMDP PREPARATIVE EXAMPLE 1.
    • CSMDP Preparative Example 4
  • The following materials were prepared: 75 g of Salvia Militiorrhiza and Panax Notoginseng extract, 7.5 g of borneol and 165 g of a mixture of cyclodextrin and agar (1:1). CSMDP was prepared by the following steps:
  • (1) Material melting step: the mixture of cyclodextrin and agar (1:1) was used as a matrix, charged into a homogenizer with the API of Compound Salvia Militiorrhiza to homogenize at 1000 rpm for 1 min to give a material; the material was molten homogenously at 3000 rpm for 1 min; during the melting process, the temperature of the material was kept at 60° C. to obtain a molten medicine liquid;
  • (2) Dropping step: the molten medicine liquid was delivered to a dripper and dropped by means of vibration dropping at the dripper temperature of 70° C. and a vibration frequency of 50 Hz under a dropping pressure of 0.5 Bar; the dropping rate was matched with the melting rate in Step (1); and,
  • (3) Condensation step: the medicine drops were cooled with a cooling gas rapidly to solidify and obtained uncoated drop pills having a particle size of 0.2 mm; the temperature of the cooling gas was 0° C.
  • The preparation method for Salvia Militiorrhiza and Panax Notoginseng extract was the same as CSMDP PREPARATIVE EXAMPLE 1.
    • CSMDP Preparative Example 5
  • The following materials were prepared: 75 g of Salvia Militiorrhiza and Panax Notoginseng extract, 7.5 g of borneol and 165 g of a mixture of arabic gum and lactose (1:1). CSMDP was prepared by the following steps:
  • (1) Material melting step: the mixture of arabic gum and lactose (1:1) was used as a matrix, charged into a homogenizer with the API of Compound Salvia Militiorrhiza to homogenize at 5000 rpm for 200 min to give a material; the material was molten homogenously at 10000 rpm for 100 min; during the melting process, the temperature of the material was kept at 100° C. to obtain a molten medicine liquid;
  • (2) Dropping step: the molten medicine liquid was delivered to a dripper and dropped by means of vibration dropping at the dripper temperature of 300° C. and a vibration frequency of 300 Hz under a dropping pressure of 4.0 Bar; the dropping rate was matched with the melting rate in Step (1); and,
  • (3) Condensation step: the medicine drops were cooled with a cooling gas rapidly to solidify and obtained uncoated drop pills having a particle size of 4.0 mm; the temperature of the cooling gas was −150° C.
  • The preparation method for Salvia Militiorrhiza and Panax Notoginseng extract was the same as CSMDP PREPARATIVE EXAMPLE 1.
    • CSMDP Preparative Example 6
  • The following materials were prepared: 75 g of Salvia Militiorrhiza and Panax Notoginseng extract, 7.5 g of borneol and 165 g of lactitol. CSMDP was prepared by the following steps:
  • (1) Material melting step: the lactitol was used as a matrix, charged into a homogenizer with the API of Compound Salvia Militiorrhiza to homogenize at 2500 rpm for 100 min to give a material; the material was molten homogenously at 6000 rpm for 50 min; during the melting process, the temperature of the material was kept at 80° C. to obtain the molten medicine liquid;
  • (2) Dropping step: the molten medicine liquid was delivered to a dripper and dropped by means of vibration dropping at the dripper temperature of 150° C. and a vibration frequency of 150 Hz under a dropping pressure of 2 Bar; the dropping rate was matched with the melting rate in Step (1);
  • (3) Condensation step: the medicine drops were cooled with a cooling gas rapidly to solidify to obtained uncoated drop pills having a particle size of 2 mm; the temperature of the cooling gas was −100° C.;
  • (4) Drying step: the resultant drop pills were dried in a fluidized state by using a fluidized drying device at 50° C. for 2 hours to give dried uncoated drop pills; and,
  • (5) Coating step: the resultant dried uncoated drop pills were coated at 40° C. in fluidized bed to obtain coated drop pills; the ratio of the coating material to the uncoated drop pills was 1:25 by weight; the concentration of the coating solution was 10 wt % and the coating material was Opadry.
  • The preparation method for Salvia Militiorrhiza and Panax Notoginseng extract was the same as CSMDP PREPARATIVE EXAMPLE 1.
    • CSMDP Preparative Example 7
  • The following materials were prepared: the API powder of Compound Salvia Militiorrhiza (including 75 g of Salvia Militiorrhiza and Panax Notoginseng extract and 7.5 g of borneol) and 165 g of PEG-8000. CSMDP was prepared by the following steps:
  • The API powder of Compound Salvia Militiorrhiza was added with water and stirred at 60° C. for 10 min or longer to obtain a pre-mixed API of Compound Salvia Militiorrhiza.
  • (1) Material melting step: the PEG-8000 and the pre-mixed API of Compound Salvia Militiorrhiza were charged into a homogenizer to homogenize at 2500 rpm for 100 min to give a material; the material was molten homogenously at 6000 rpm for 50 min; during the melting process, the temperature of the material was kept at 80° C. to obtain a molten medicine liquid;
  • (2) Dropping step: the molten medicine liquid was delivered to a dripper and dropped by means of vibration dropping at a dripper temperature of 150° C. and a vibration frequency of 150 Hz under a dropping pressure of 2 Bar; the dropping rate was matched with the melting rate in Step (1);
  • (3) Condensation step: the medicine drops were cooled with a cooling gas rapidly to solidify and obtained uncoated drop pills having a particle size of 2 mm; the temperature of the cooling gas was −100° C.;
  • (4) Drying step: the resultant drop pills were dried in a fluidized state at 50° C. for 2 hours to give the dried uncoated drop pill; and,
  • (5) Coating step: the resultant dried uncoated drop pills were coated at 40° C. in fluidized bed to obtain coated drop pills; the ratio of the coating material to the dried uncoated drop pills was 1:25 by weight; the concentration of the coating solution was 10 wt % and the coating material was shellac.
  • The preparation method for Salvia Militiorrhiza and Panax Notoginseng extract was the same as CSMDP PREPARATIVE EXAMPLE 1.
    • CSMDP Preparative Example 8
  • The following materials were prepared: the API powder of Compound Salvia Militiorrhiza (including 90 g of Salvia Militiorrhiza and Panax Notoginseng extract and 2 g of borneol) and 270 g of PEG-1000. CSMDP was prepared by the following steps:
  • The API powder of Compound Salvia Militiorrhiza was added with water and stirred at 30° C. for 10 min or longer to obtain a pre-mixed API of Compound Salvia Militiorrhiza.
  • (1) Material melting step: the PEG-1000 and the pre-mixed API of Compound Salvia Militiorrhiza were charged into a homogenizer to homogenize at 2500 rpm for 100 min to give a material; the material was molten homogenously at 6000 rpm for 20 min; during the melting process, the temperature of the material was kept at 100° C. to obtain a molten medicine liquid;
  • (2) Dropping step: the molten medicine liquid was delivered to a dripper and dropped by means of vibration dropping at a dripper temperature of 70° C. and a vibration frequency of 100 Hz under a dropping pressure of 1.0 Bar and an acceleration speed of 1G and a dropping rate of 10 Kg/h; the dropping rate was matched with the melting rate in Step (1);
  • (3) Condensation step: the medicine drops were cooled with a cooling gas rapidly to solidify and obtained uncoated drop pills having a particle size of 2 mm; the temperature of the cooling gas was −80° C.;
  • (4) Drying step: the resultant drop pills were dried by a gradient-rising temperature drying method, fluidized at −20° C., dried at 15° C. for 10 min, further dried at 35° C. for 10 min, and further dried at 55° C. for 30 min to give dried uncoated drop pills; and,
  • (5) Coating step: the resultant dried uncoated drop pills were coated at 40° C. in a fluidized bed to obtain coated drop pills; the ratio of the coating material to the dried uncoated drop pills was 1:25 by weight; the concentration of the coating solution was 10 wt % and the coating material was cellulose acetate phthalate (CAP).
  • The preparation method for Salvia Militiorrhiza and Panax Notoginseng extract was the same as CSMDP PREPARATIVE EXAMPLE 1.
    • CSMDP Preparative Example 9
  • The following materials were prepared: the API powder of Compound Salvia Militiorrhiza (including 100 g of Salvia Militiorrhiza and Panax Notoginseng extract and 5 g of borneol) and 35 g of a mixture of PEG-4000:PEG-6000 (1:1). CSMDP was prepared by the following steps:
  • The API powder of Compound Salvia Militiorrhiza was added with water and stirred at 80° C. for 10 min or longer to obtain a pre-mixed API of Compound Salvia Militiorrhiza.
  • (1) Material melting step: the mixture of PEG-4000:PEG-6000 (1:1) and the pre-mixed API of Compound Salvia Militiorrhiza were charged into a homogenizer to homogenize at 2500 rpm for 100 min to give a material; the material was molten homogenously at 6000 rpm for 80 min; during the melting process, the temperature of the material was kept at 80° C. to obtain a molten medicine liquid;
  • (2) Dropping step: the molten medicine liquid was delivered to a dripper and dropped by means of vibration dropping at a dripper temperature of 100° C. and a vibration frequency of 200 Hz under a dropping pressure of 3.0 Bar and a acceleration speed of 20G and a dropping rate of 40 Kg/h; the dropping rate was matched with the melting rate in Step (1);
  • (3) Condensation step: the medicine drops were cooled with a cooling gas rapidly to solidify and obtained uncoated drop pills having a particle size of 2 mm; the temperature of the cooling gas was −120° C.;
  • (4) Drying step: the resultant drop pills were dried by a gradient-rising temperature drying method, fluidized at 30° C., dried at 35° C. for 120 min, at 55° C. for 60 min and at 100° C. for 60 min to give dried uncoated drop pills; and,
  • (5) Coating step: the resultant dried uncoated drop pills were coated at 35° C. in a fluidized bed to obtain coated drop pills; the ratio of the coating material to the dried uncoated drop pills was 1:25 by weight; the concentration of the coating solution was 10 wt % and the coating material was methyl acrylate.
  • The preparation method for Salvia Militiorrhiza and Panax Notoginseng extract was the same as CSMDP PREPARATIVE EXAMPLE 1.
    • CSMDP Preparative Example 10
  • The following materials were prepared: 600 g of Salvia Militiorrhiza and Panax Notoginseng extract, 5 g of borneol and 600 g of xylitol as the drop pill matrix. CSMDP was prepared by the following steps:
  • (1) Material melting step: the xylitol was firstly charged into a melting tank and heated to 90° C. to pre-melt, into which the API of Compound Salvia Militiorrhiza was charged and well mixed to give a molten medicine liquid;
  • (2) Dropping step: the molten medicine liquid was delivered under pressure to a dripper that was heat-insulated by a steam jacket; at the dripper temperature of 40° C. and a vibration frequency for dropping of 50 Hz, the molten medicine liquid was flowed into the dripper and obtained drops from the bottom of the dripper;
  • (3) Condensation step: the medicine drops were cooled in a cooling duct with low-temperature inert gas to condensation to obtain solid drop pills; the cooling temperature was −20° C.;
  • (4) Drying & coating step: the resultant solid drop pills were dried in a fluidized state and drug-loading coated to give coated micro drop pills with a particle size of 0.2 mm˜1.0 mm; the drying temperature was 75° C.; and,
  • (5) Packaging step: the coated micro drop pills with a particle size of 0.2 mm˜1.0 mm were loaded into capsules; 100% of the capsules were on-line checkweighed with a capsule checkweigher and packaged to give the final product.
  • The preparation method for Salvia Militiorrhiza and Panax Notoginseng extract was the same as CSMDP PREPARATIVE EXAMPLE 1.
  • Wherein, during the dropping process, the formation of drop pills was measured visually by using a stroboscopic illumination to perform real-time monitoring and adjustment. After the drug-loading coating, in order to improve the uniformity and roundness of the drop pills, the steps of screening and regulating the drop pills could be added.
    • CSMDP Preparative Example 11
  • The following materials were prepared: 600 g of Salvia Militiorrhiza and Panax Notoginseng extract, 5 g of borneol and 3000 g of a mixture of PEG-6000 and PEG-4000 as the drop pill matrix. CSMDP was prepared by the following steps:
  • (1) Material melting step: the mixture of PEG-6000 and PEG-4000 was firstly charged into a melting tank and pre-molten by heating to 120° C., into which the API of Compound Salvia Militiorrhiza was charged and well mixed to give a molten medicine liquid;
  • (2) Dropping step: the molten medicine liquid was delivered under pressure to a dripper that was heat-insulated by a steam jacket; at a dripper temperature of 80° C. and a vibration frequency for dropping of 20 Hz, the molten medicine liquid was flowed into the dripper and obtained medicine drops from the bottom of the dripper;
  • (3) Condensation step: the medicine drops were cooled with low-temperature inert gas to condensation to obtain solid drop pills; the cooling temperature was −80° C.;
  • (4) Drying & coating step: the resultant solid drop pills were dried in a fluidized state and drug-loading coated to give coated micro drop pills with a particle size of 0.5 mm˜1.0 mm; the drying temperature was 150° C.; and,
  • (5) Packaging step: the micro drop pills were loaded into capsules; 100% of the capsules were on-line checkweighed with a capsule checkweigher and packaged to give the final product.
  • The preparation method for Salvia Militiorrhiza and Panax Notoginseng extract was the same as CSMDP PREPARATIVE EXAMPLE 1.
  • Wherein, during the dropping process, the formation of drop pills was measured visually by using a stroboscopic illumination to perform real-time monitoring and adjustment. After the drug-loading coating, in order to improve the uniformity and roundness of the drop pills, the step of screening and regulating the drop pills could be added.
    • CSMDP Preparative Example 12
  • The following materials were prepared: 600 g of Salvia Militiorrhiza and Panax Notoginseng extract, 5 g of borneol and 120 g of PEG-1000 as the drop pill matrix. CSMDP was prepared by the following steps:
  • (1) Material melting step: the PEG-1000 was firstly charged into a melting tank and pre-molten by heating to 40° C., into which the API of Compound Salvia Militiorrhiza was charged and well mixed to give a molten medicine liquid;
  • (2) Dropping step: the molten medicine liquid was delivered under pressure to a dripper that was heat-insulated by a steam jacket; at a dripper temperature of 40˜60° C. and a vibration frequency for dropping of 200 Hz, the molten medicine liquid was flowed into the dripper and obtained medicine drops from the bottom of the dripper;
  • (3) Condensation step: the medicine drops were cooled with low-temperature inert gas to condensation to obtain solid drop pills; the cooling temperature was −100° C.;
  • (4) Drying & coating step: the resultant solid drop pills were dried in a fluidized state and drug-loading coated, fluidized at 20° C., dried at 25° C. for 60 min, further dried at 45° C. for 30 min and at 55° C. for 30 min to give the coated micro drop pill with a particle size of 3.0 mm˜4.0 mm; and,
  • (5) Packaging step: the micro drop pills were loaded into capsules; 100% of the capsules were on-line checkweighed with a capsule checkweigher and packaged to give the final product.
  • The preparation method for Salvia Militiorrhiza and Panax Notoginseng extract was the same as CSMDP PREPARATIVE EXAMPLE 1.
  • Wherein, during the dropping process, the formation of drop pills was measured visually by using a stroboscopic illumination to perform real-time monitoring and adjustment. In order to improve the uniformity and roundness of the drop pills, the step of screening and regulating the drop pills could be added.
    • CSMDP Preparative Example 13
  • The following materials were prepared: 600 g of Salvia Militiorrhiza and Panax Notoginseng extract, 5 g of borneol and 3000 g of a mixture of PEG-6000 and PEG-4000 as the drop pill matrix. CSMDP was prepared by the following steps:
  • (1) Material melting step: the mixture of PEG-6000 and PEG-4000 was firstly charged into a melting tank and pre-molten by heating to 120° C., into which the API of Compound Salvia Militiorrhiza was charged into a homogenizer to homogenize at 1000 rpm for 1 min and molten homogenously at 3000 rpm for 1 min, during the melting process, the temperature of the material was kept at 60° C. to obtain a molten medicine liquid;
  • (2) Dropping step: the molten medicine liquid was delivered under pressure to a dripper that was heat-insulated by a steam jacket; at a dripper temperature of 70° C., a vibration frequency for dropping of 50 Hz and a dropping pressure of 0.5 Bar, the molten medicine liquid was flowed into the dripper and obtained medicine drops from the bottom of the dripper;
  • (3) Condensation step: the medicine drops were cooled with low-temperature inert gas to condensation to obtain solid drop pills; the cooling temperature was 0° C.;
  • (4) Drying & coating step: the resultant solid drop pills were dried in a fluidized state and drug-loading coated to give coated micro drop pills with a particle size of 0.2 mm; the drying temperature was 150° C.; and,
  • (5) Packaging step: the micro drop pills were loaded into capsules; 100% of the capsules were on-line checkweighed with a capsule checkweigher and packaged to give the final product.
  • The preparation method for Salvia Militiorrhiza and Panax Notoginseng extract was the same as CSMDP PREPARATIVE EXAMPLE 1.
    • CSMDP Preparative Example 14
  • The following materials were prepared: 600 g of Salvia Militiorrhiza and Panax Notoginseng extract, 5 g of borneol and 1800 g of PEG-6000 as the drop pill matrix. CSMDP was prepared by the following steps:
  • (1) Material melting step: the PEG-6000 was firstly charged into a melting tank and pre-molten by heating to 120° C., into which the API of Compound Salvia Militiorrhiza was charged into a homogenizer to homogenize at 5000 rpm for 200 min and molten homogenously at 10000 rpm for 1 min, during the melting process, the temperature of the material was kept at 100° C. to obtain a molten medicine liquid;
  • (2) Dropping step: the molten medicine liquid was delivered under pressure to a dripper that was heat-insulated by a steam jacket; at a dripper temperature of 300° C., a vibration frequency of 300 Hz and a dropping pressure of 4.0 Bar, the molten medicine liquid was flowed into the dripper and obtained medicine drops from the bottom of the dripper;
  • (3) Condensation step: the medicine drops were cooled with low-temperature inert gas to condensation to obtain solid drop pills; the cooling temperature was −150° C.;
  • (4) Drying & coating step: the resultant solid drop pills were dried in a fluidized state and drug-loading coated to give coated micro drop pills with a particle size of 4.0 mm; the drying temperature was 150° C.; and,
  • (5) Packaging step: the micro drop pills were loaded into capsules; 100% of the capsules were on-line checkweighed with a capsule checkweigher and packaged to give the final product.
  • The preparation method for Salvia Militiorrhiza and Panax Notoginseng extract was the same as CSMDP PREPARATIVE EXAMPLE 1.
    • CSMDP Preparative Example 15
  • The following materials were prepared: 600 g of Salvia Militiorrhiza and Panax Notoginseng extract, 5 g of borneol and 2400 g of PEG-4000 as the drop pill matrix. CSMDP was prepared by the following steps:
  • (1) Material melting step: the PEG-4000 was firstly charged into a melting tank and pre-molten by heating to 120° C., into which the API of Compound Salvia Militiorrhiza was charged, homogenized at 3000 rpm for 10 min and molten homogenously at 4000 rpm for 5 min, during the melting process, the temperature of the material was kept at 70˜90° C. to obtain a molten medicine liquid;
  • (2) Dropping step: the molten medicine liquid was delivered under pressure to a dripper that was heat-insulated by a steam jacket; at a dripper temperature of 70° C., a vibration frequency for dropping of 90 Hz and a dropping pressure of 1.0 Bar, the molten medicine liquid was flowed into the dripper and obtained medicine drops from the bottom of the dripper;
  • (3) Condensation step: the medicine drops were cooled with low-temperature inert gas to condensation to obtain solid drop pills; the cooling temperature was −140° C.; and,
  • (4) Drying step: the resultant solid drop pills were dried in a fluidized state to give uncoated micro drop pills with a particle size of 1.0 mm; the drying temperature was 150° C.
  • The preparation method for Salvia Militiorrhiza and Panax Notoginseng extract was the same as CSMDP PREPARATIVE EXAMPLE 1.
    • CSMDP Preparative Example 16
  • The following materials were prepared: 600 g of Salvia Militiorrhiza and Panax Notoginseng extract, 5 g of borneol and 2400 g of PEG-4000 as the drop pill matrix. CSMDP was prepared by the following steps:
  • (1) Material melting step: the PEG-4000 was firstly charged into a melting tank and pre-molten by heating to 120° C., into which the API of Compound Salvia Militiorrhiza was charged, homogenized at 4000 rpm for 60 min and molten homogenously at 9000 rpm for 30 min, during the melting process, the temperature of the material was kept at 90° C. to obtain a molten medicine liquid;
  • (2) Dropping step: the molten medicine liquid was delivered under pressure to a dripper that was heat-insulated by a steam jacket; at a dripper temperature of 100° C., a vibration frequency for dropping of 200 Hz and a dropping pressure of 3.0 Bar, the molten medicine liquid was flowed into the dripper and obtained medicine drops from the bottom of the dripper;
  • (3) Condensation step: the medicine drops were cooled with low-temperature inert gas to condensation to obtain solid drop pills; the cooling temperature was −140° C.; and,
  • (4) Drying step: the resultant solid drop pills were dried in a fluidized state to give uncoated micro drop pills with a particle size of 2.0 mm; the drying temperature was 150° C.
  • The preparation method for Salvia Militiorrhiza and Panax Notoginseng extract was the same as CSMDP PREPARATIVE EXAMPLE 1.
    • CSMDP Preparative Example 17
  • The following materials were prepared: 600 g of Salvia Militiorrhiza and Panax Notoginseng extract, 5 g of borneol and 2000 g of PEG-6000 as the drop pill matrix. CSMDP was prepared by the following steps:
  • (1) Material melting step: the PEG-6000 was firstly charged into a melting tank and pre-molten by heating to 90° C., into which the API of Compound Salvia Militiorrhiza was charged and well mixed to give a molten medicine liquid;
  • (2) Dropping step: the molten medicine liquid was delivered under pressure to a dripper that was heat-insulated by a steam jacket; at dripper temperature of 80° C. and a vibration frequency for dropping of 50 Hz, the molten medicine liquid was flowed into the dripper and obtained medicine drops from the bottom of the dripper;
  • (3) Condensation step: the medicine drops were cooled with low-temperature inert gas to condensation to obtain solid drop pills; the cooling temperature was −20° C.;
  • (4) Drying & coating step: the resultant solid drop pills were dried in a fluidized state and drug-loading coated to give coated micro drop pills with a particle size of 1.0 mm˜2.0 mm; the drying temperature was 75° C.; and,
  • (5) Packaging step: the coated micro drop pills were loaded into capsules; 100% of the capsules were on-line checkweighed with a capsule checkweigher and packaged to give the final product.
  • The preparation method for Salvia Militiorrhiza and Panax Notoginseng extract was the same as CSMDP PREPARATIVE EXAMPLE 1.
  • Wherein, during the dropping process, the formation of drop pills was measured visually by using a stroboscopic illumination to perform real-time monitoring and adjustment. In order to improve the uniformity and roundness of the drop pills, the step of screening and regulating the drop pills could be added.
  • As found by the study of the inventors, compared with the current CSDP, the CSMDP prepared by the methods disclosed in the CSMDP PREPARATIVE EXAMPLES 2˜17 had the similar merits such as high bioavailability, reduced administration dosage and good compliance to the patients. Meanwhile, the CSMDP prepared by the methods disclosed in CSMDP PREPARATIVE EXAMPLE 2˜17 had the same merits listed in Table 2.
    • Example 2 QMDP (Qishenyiqi Micro Drop Pill)
  • Qishenyiqi drop pill is a TCM preparation prepared by Astragalus membranaceus, Salvia Militiorrhiza, Panax Notoginseng and volatile oil from Lignum Dalbergiae Odoriferae. It is capable of significantly improving symptoms such as myocardial injury and heart dysfunction, which has been used clinically for treating diseases of chronic heart failure, myocarditis and its sequelae, myocardial infarction recovery stage and myocardial fibrosis. The current Qishenyiqi drop pill has the merits such as small dosage, convenient administration, rapid dissolution, direct absorption into blood by mucosa, high bioavailability and high efficacy with no gastrointestinal stimulation and no obvious toxic and side effects.
  • The preparation method for QMDP known in the prior art mainly comprises the following steps: firstly, the following crude drugs were prepared: Astragalus membranaceus, Salvia Militiorrhiza, Panax Notoginseng, volatile oil from Lignum Dalbergiae Odoriferae and PEG-6000; Salvia Militiorrhiza and Panax Notoginseng were decocted with water and precipitated with ethanol; the ethanol was recovered and concentrated to obtain the Salvia Militiorrhiza and Panax Notoginseng extract; Astragalus membranaceus was decocted with water and precipitated with ethanol to obtain deposit of Astragalus membranaceus; Lignum Dalbergiae Odoriferae was extracted with water to obtain volatile oil from Lignum Dalbergiae Odoriferae; the Salvia Militiorrhiza and Panax Notoginseng extract, the deposit of Astragalus membranaceus and PEG-6000 were well molten on a water bath, followed by addition of volatile oil from Lignum Dalbergiae Odoriferae and well mixed and delivered to a dripping machine to prepare drop pills. Although the method was very mature for preparing Qishenyiqi drop pills in the prior art, there were still problems faced during preparation process, e.g. a large amount of the matrix and a small unit drug-loading capacity.
  • In the present invention, Qishenyiqi micro drop pills are prepared by the API and the drop pill matrix in a ratio of 1:5˜5:1 by weight. The API is prepared by the following crude drugs by weight parts:
  • Astragalus membranaceus 100˜200 parts;
  • Salvia Militiorrhiza 50˜100 parts;
  • Panax Notoginseng 10˜20 parts; and,
  • Volatile oil from Lignum Dalbergiae Odoriferae 0.5˜2 parts.
  • Preferably, the API is prepared by the following crude drugs by weight parts:
  • Astragalus membranaceus 150˜180 parts;
  • Salvia Militiorrhiza 75˜85 parts;
  • Panax Notoginseng 13˜18 parts; and,
  • Volatile oil from Lignum Dalbergiae Odoriferae 0.5˜1 parts.
  • Most preferably, the API is prepared by the following crude drugs by weight parts:
  • Astragalus membranaceus 150 parts;
  • Salvia Militiorrhiza 75 parts;
  • Panax Notoginseng 15 parts; and,
  • Volatile oil from Lignum Dalbergiae Odoriferae 1 part.
  • Preferably, the micro drop pills are prepared by the API and the drop pill matrix in a ratio of 1:3˜3:1 by weight, most preferably 1:(1˜3) by weight.
  • In the present invention, the API of Qishenyiqi micro drop pill is used as the active pharmaceutical ingredient, which is prepared by the following steps: Astragalus membranaceus, Salvia Militiorrhiza and Panax Notoginseng were extracted and followed by addition of volatile oil from Lignum Dalbergiae Odoriferae. The preparation of the API belongs to the prior art, and the API can be prepared by the conventional methods with the crude drugs in the ratios of the present invention, or by the commercially available Astragalus membranaceus extract, Salvia Militiorrhiza extract, Panax Notoginseng extract and volatile oil from Lignum Dalbergiae Odoriferae. In order to better achieve the present invention, the API is preferably prepared by the following method:
  • (1) Decocting Salvia Militiorrhiza and Panax Notoginseng with water under an alkaline condition to give a decoction, filtering the decoction, concentrating and precipitating the filtrate with ethanol to get a supernatant, filtering the supernatant, recovering ethanol and concentrating to give the Salvia Militiorrhiza and Panax Notoginseng extract;
  • (2) Decocting Astragalus membranaceus under an alkaline condition to give a decoction, filtering the decoction, concentrating and precipitating the filtrate with ethanol, filtering the supernatant, recovering ethanol and concentrating to give the Astragalus membranaceus extract;
  • (3) Mixing the Astragalus membranaceus extract and Salvia Militiorrhiza and Panax Notoginseng extract and then adding the volatile oil from Lignum Dalbergiae Odoriferae to give the API.
  • Preferably in Step (1), under an alkaline condition, Salvia Militiorrhiza and Panax Notoginseng are decocted with water for 1˜3 times, 1˜3 hours each time to give a decoction, and the decoction was filtered to get a filtrate; the filtrate is concentrated to give a concentrated liquid, into which 70˜100% (v/v) ethanol is added to make the final concentration of ethanol 50˜70% (v/v) and allow to stand still to get a supernatant; the supernatant is taken, filtered, ethanol is recovered and concentrated to give the Salvia Militiorrhiza and Panax Notoginseng extract. Most preferably, Salvia Militiorrhiza and Panax Notoginseng are decocted with water and an appropriate amount of alkali for 2 times, 2 hours each time and filtered to get a filtrate for each decoction; the filtrates are combined and concentrated to give a concentrated liquid with a relative density of 1.13˜1.23 (80° C.), into which ethanol is added to make a final concentration of ethanol 65˜70% (v/v) and allow to stand still for 12 hours or longer to get a supernatant; the supernatant is filtered, ethanol is recovered and concentrated to give the Salvia Militiorrhiza and Panax Notoginseng extract with a relative density of 1.30˜1.38 (80° C.).
  • In Step (2), Astragalus membranaceus is decocted with an alkaline aqueous solution for 1˜3 times, 1˜3 hours each time, to give a decoction; the decoction is filtered to give Filtrate I; dregs of the decoction is further decocted with water for 1˜3 times, 1˜3 hours each time, to give a decoction; the decoction is filtered to give Filtrate II; Filtrate I and Filtrate II are combined and concentrated to give a concentrated liquid, into which 50˜100% (v/v) ethanol is added to perform ethanol precipitation for 1˜3 times to make the final concentration of ethanol 60˜80% (v/v) and allow to stand still to get a supernatant; the supernatant is filtered to give Filtrate III; Filtrate III is recovered and concentrated by ethanol to give the Astragalus membranaceus extract.
  • Most preferably, in Step (2), Astragalus membranaceus is decocted with water and an appropriate amount of sodium bicarbonate for 2 hours to give a decoction; the decoction was filtered to give Filtrate I; dregs of the decoction is further decocted with water for 1 hour to give a decoction; the decoction is filtered to give Filtrate II; Filtrate I and Filtrate II are combined and concentrated to give a concentrated liquid with a relative density 1.05˜1.20 (75±5° C.), ethanol is added into the concentrated liquid to make the final concentration of ethanol 60±1% (v/v) and allow to stand still for 12 hours or longer to get a supernatant, the supernatant is filtered and recovered ethanol under a reduced pressure to obtain a concentrated liquid with a relative density of 1.18˜1.30 (60±5° C.), into which ethanol is added to make the final concentration of ethanol 80±1% (v/v) and allow to stand still for 12 hours or longer to get a supernatant; the supernatant is filtered and concentrated by recovering ethanol under a reduced pressure to give the Astragalus membranaceus extract with a relative density of 1.30˜1.38 (70±5° C.).
  • The alkaline condition is at a pH value of 7.5˜9.0 and the alkali is, but not limited to, selected from the group consisting of sodium bicarbonate, sodium carbonate, disodium hydrogen phosphate, sodium dihydrogen phosphate, sodium hydroxide, potassium hydroxide and magnesium hydroxide.
  • The preparation method for preparing the QMDP comprises the following steps:
  • (1) Material melting step: charging the API and the drop pill matrix in a ratio of 1:5˜5:1 by weight into a homogenizer, mixing homogenously at 1000˜5000 rpm for 1˜200 min, melting homogenously at 3000˜10000 rpm for 1˜100 min; during the melting process, the temperature of the material is kept at 60˜100° C. to obtain a molten medicine liquid;
  • (2) Dropping step: delivering the molten medicine liquid to a dripper at 70° C.˜−300° C., and acquiring medicine drops by means of vibration dropping at a vibration frequency of 50˜300 Hz under a dropping pressure of 0.5˜4.0 Bar; the dropping rate is matched with the melting rate in Step (1);
  • (3) Condensation step: cooling the medicine drops with a cooling gas rapidly to solidify and obtaining solid uncoated drop pills having a particle size of 0.2 mm˜-4.0 mm; the temperature of the cooling gas is 0° C.˜−150° C.
  • After Step (2) and Step (3), the pill weight decreased from 23.5˜27.5 mg of the traditional drop pills to 3˜5 mg, which can be loaded into capsules; the use of gas cooling can solve the problems such as residual coolant of liquid paraffin in the current drop pills.
    • QMDP Preparative Example 1
  • The following materials were prepared: 80 g of the API of QMDP and 165 g of PEG-6000.
  • (1) Pre-mixing step: the API of QMDP was added with water to pre-mix, stirred in a heat-insulated tank at 40±10° C. for 60 min or longer to make the water content of API of QMDP at 13.0 wt % to give a pre-mixed API of QMDP for later use;
  • (2) Material melting step: the PEG-6000 was firstly added into a melting tank, pre-molten by heating to 90° C., into which the pre-mixed API of QMDP was added, and the resultant material was mixed by a low-speed homogenization (3200 rpm); after mixing, the homogenization rate was increased to 5000 rpm to melt for 6 min; during melting process, the temperature of the material was kept at 80±5° C. to give a molten medicine liquid;
  • (3) Dropping step: the molten medicine liquid was delivered to a dripper, the vibration frequency of the dripper was adjusted to 137 Hz and the temperature of the dripper was controlled at 80° C.; the molten medicine liquid was flowed into the dripper under pressure (a pressure for dropping is at 0.18 Bar), and obtained medicine drops from the bottom of the dripper;
  • (4) Condensation step: the medicine drops were cooled in a cooling duct with low-temperature inert gas at −115±5° C. to cool the liquid to form solid drop pills;
  • (5) Drying step: the resultant drop pills were dried in a fluidized state; until the drop pills reached a better fluidization state in the bed of the fluidized bed, the temperature was increased to 25° C. to dry for 60 min, further increased to 45° C. to dry for 30 min, continuously increased to 55° C. to dry for 30 min, and deceased 30° C. or lower to discharge to give uncoated drop pills as a intermediate product, and the water content of the uncoated drop pills was controlled in a range of 3.0˜7.0 wt %;
  • (6) Coating step: the amount of coating powder was calculated based on the coating feed capacity and formulation; Opadry, which has 4 wt % of the weight of the uncoated drop pills, was used to prepare a 18 wt % coating solution and stirred for 45 min; the inlet air temperature was initially set to 25° C.; after the qualified uncoated drop pills were loaded into the fluidized bed, the inlet air temperature was increased to 48° C.; until the temperature of the drop pills was up to 38° C., the coating was started; the temperature of the material was kept in the range of 35˜45° C. during the coating and decreased 30° C. or lower after coating; the drop pills were discharged, screened to give coated drop pills as a intermediate product, the coating weigh of the coated drop pills was controlled in a range of 3.3±0.7% and the water content was controlled in a range of 3.0˜7.0 wt %; and,
  • (7) Loading into capsule and packaging step: the resultant micro drop pills with a particle size of 1.0 mm˜2.0 mm were loaded into capsules; 100% of the capsules were on-line checkweighed with a capsule checkweigher, packaged to give the final product.
  • Wherein, during the dropping process, the formation of the drop pills was measured visually by using a stroboscopic illumination to perform a real-time monitoring and adjustment. In order to improve the uniformity and roundness of the drop pills, the steps of screening and regulating the drop pills could be added.
  • Further, the API of QMDP was prepared by the following method:
  • (1) 75 weight parts of Salvia Militiorrhiza and 15 weight parts of Panax Notoginseng were decocted with water under an alkaline condition to give a decoction; the decoction was filtered, concentrated and precipitated with ethanol to get a supernatant; the supernatant was filtered, recovered ethanol and concentrated to give a Salvia Militiorrhiza and Panax Notoginseng extract;
  • (2) 150 weight parts of Astragalus membranaceus was decocted with an alkaline aqueous solution to give a decoction; the decoction was filtered, concentrated and precipitated with ethanol to get a supernatant; the supernatant was filtered, recovered ethanol and concentrated to give a Astragalus membranaceus extract;
  • (3) the Astragalus membranaceus extract and the Salvia Militiorrhiza and Panax Notoginseng extract were well mixed, and 1 weight part of volatile oil from Lignum Dalbergiae Odoriferae was added to give the API.
  • Wherein, in Step (1), Salvia Militiorrhiza and Panax Notoginseng were decocted with water and an appropriate amount of alkali for 2 times, 2 hours each time to give a decoction, and the decoction was filtered to get filtrates; the filtrates were combined and concentrated to give a concentrated liquid with a relative density of 1.13˜1.23(80° C.); ethanol was added into the concentrated liquid to make a final concentration of ethanol 65˜70% (v/v) and allowed to stand still for 12 hours or longer to get a supernatant; the supernatant was filtered, and the ethanol therein was recovered and concentrated to give the Salvia Militiorrhiza and Panax Notoginseng extract with a relative density of 1.30˜1.38(80° C.).
  • Wherein, in Step (2), Astragalus membranaceus is decocted with water and an appropriate amount of sodium bicarbonate for 2 hours to give a decoction; the decoction was filtered to give Filtrate I; dregs of the decoction is further decocted with water for 1 hour to give a decoction; the decoction is filtered to give Filtrate II; Filtrate I and Filtrate II are combined and concentrated to give a concentrated liquid with a relative density 1.05˜1.20 (75±5° C.), ethanol is added into the concentrated liquid to make the final concentration of ethanol 60±1% (v/v) and allow to stand still for 12 hours or longer to get a supernatant, the supernatant is filtered and recovered ethanol under a reduced pressure to obtain a concentrated liquid with a relative density of 1.18˜1.30 (60±5° C.), into which ethanol is added to make the final concentration of ethanol 80±1% (v/v) and allow to stand still for 12 hours or longer to get a supernatant; the supernatant is filtered and concentrated by recovering ethanol under a reduced pressure to give the Astragalus membranaceus extract with a relative density of 1.30˜1.38 (70±5° C.).
  • The volatile oil from Lignum Dalbergiae Odoriferae was commercially available.
    • QMDP Preparative Example 2
  • The following materials were prepared: 100 g of Salvia Militiorrhiza and Panax Notoginseng extract, 200 g of Astragalus membranaceus extract, 10 g of volatile oil from Lignum Dalbergiae Odoriferae and 900 g of PEG-6000 as the drop pill matrix.
  • (1) Material melting step: the PEG-6000 was loaded into a melting tank and pre-molten by heating to 70˜80° C., into which a uniform mixture of the Salvia Militiorrhiza and Panax Notoginseng extract and the Astragalus membranaceus extract as well as volatile oil from Lignum Dalbergiae Odoriferae were added, mixed and homogenized to give a molten medicine liquid;
  • (2) Dropping step: the molten medicine liquid was delivered to a dripper and dropped by means of vibration dropping at a dripper temperature of 80° C. and a vibration frequency of 50 Hz; the dropping rate was matched with the melting rate in Step (1); and,
  • (3) Condensation step: the medicine drops were cooled with a cooling gas rapidly to solidify and obtained solid drop pills; the cooling gas was low-temperature nitrogen at −40° C.;
  • (4) Drying & coating step: the resultant drop pills was dried in a fluidized state and drug-loading coated at 150° C., screened, regulated and packaged to obtain the final product.
    • QMDP Preparative Example 3
  • Except that the API of QMDP was prepared by the following crude drugs by weight parts: Astragalus membranaceus 100 parts, Salvia Militiorrhiza 50 parts, Panax Notoginseng 10 parts, volatile oil from Lignum Dalbergiae Odoriferae 0.5 parts, and the ratio of the API of QMDP to PEG-6000 was 1:5 by weight, the Qishenyiqi micro drop pills were prepared by the same method as QMDP PREPARATIVE EXAMPLE 1.
    • QMDP Preparative Example 4
  • Except that the API of QMDP was prepared by the following crude drugs by weight parts: Astragalus membranaceus 200 parts, Salvia Militiorrhiza 100 parts, Panax Notoginseng 20 parts, volatile oil from Lignum Dalbergiae Odoriferae 2 parts, and the ratio of the API of QMDP to PEG-6000 was 5:1 by weight, the Qishenyiqi micro drop pills were prepared by the same method as QMDP PREPARATIVE EXAMPLE 1.
    • QMDP Preparative Example 5
  • The following materials were prepared: 80 g of the API of QMDP, 165 g of a cyclodextrin and agar (1:1) mixture. The QMDP was prepared by the following method:
  • (1) Material melting step: the cyclodextrin and agar (1:1) mixture was charged into a homogenizer with the API of QMDP to homogenize at 1000 rpm for 1 min to give a material; the material was molten homogenously at 3000 rpm for 1 min; during the melting process, the temperature of the material was kept at 60° C. to obtain a molten medicine liquid;
  • (2) Dropping step: the molten medicine liquid was delivered to a dripper and dropped by means of vibration dropping at a dripper temperature of 70° C. and a vibration frequency of 50 Hz under a dropping pressure of 0.5 Bar; the dropping rate was matched with the melting rate in Step (1); and,
  • (3) Condensation step: the medicine drops were cooled with a cooling gas rapidly solidify and obtained uncoated drop pills having a particle size of 0.2 mm; the temperature of the cooling gas was 0° C.
    • QMDP Preparative Example 6
  • The following materials were prepared: 80 g of the API of QMDP, 165 g of arabic gum and lactose (1:1) mixture. The QMDP was prepared by the following method:
  • (1) Material melting step: the arabic gum and lactose (1:1) mixture was charged into a homogenizer with the API of QMDP to homogenize at 5000 rpm for 200 min to give a material; the material was molten homogenously at 10000 rpm for 100 min; during the melting process, the temperature of the material was kept at 100° C. to obtain a molten medicine liquid;
  • (2) Dropping step: the molten medicine liquid was delivered to a dripper and dropped by means of vibration dropping at a dripper temperature of 300° C. and a vibration frequency of 300 Hz under a dropping pressure of 4.0 Bar; the dropping rate was matched with the melting rate in Step (1); and,
  • (3) Condensation step: the medicine drops were cooled with a cooling gas rapidly to solidify and obtained uncoated drop pills having a particle size of 4.0 mm; the temperature of the cooling gas was −150° C.
    • QMDP Preparative Example 7
  • The following materials were prepared: 80 g of the API of QMDP and 165 g of lactitol. The QMDP was prepared by the following method:
  • (1) Material melting step: the API of QMDP and lactitol were loaded into a homogenizer to homogenize at 2500 rpm for 100 min and molten homogenously at 6000 rpm for 50 min to give a molten medicine liquid; during the melting process, the temperature of the material was kept at 80° C.;
  • (2) Dropping step: the molten medicine liquid was delivered to a dripper and dropped by means of vibration dropping at a dripper temperature of 150° C. and a vibration frequency of 150 Hz under a dropping pressure of 2 Bar; the dropping rate was matched with the melting rate in Step (1); and,
  • (3) Condensation step: the medicine drops were cooled with a cooling gas rapidly to solidify and obtained the solid uncoated drop pills having a particle size of 2 mm; the temperature of the cooling gas was at −100° C.;
  • (4) Drying step: the resultant drop pills were dried in a fluidized state by using a fluidized drying device at 50° C. for 2 hours to give dried uncoated drop pills; and,
  • (5) Coating step: the uncoated drop pills were coated at 45° C. on a fluidized bed to give coated drop pills, the ratio of the coating material of shellac to the uncoated drop pills was 1:25 by weight, the coating solution is at 10 wt %.
    • QMDP Preparative Example 8
  • The following materials were prepared: 80 g of the API of QMDP powder and 165 g of PEG-8000. The QMDP was prepared by the following method:
  • The API of QMDP powder was added with water and stirred at 60° C. for 10 min or longer to give a pre-mixed material.
  • (1) Material melting step: the pre-mixed material and PEG-8000 were loaded into a homogenizer to homogenize at 2500 rpm for 100 min and molten homogenously at 6000 rpm for 50 min to give a molten medicine liquid; during the melting process, the temperature of the material was kept at 80° C.;
  • (2) Dropping step: the molten medicine liquid was delivered to a dripper and dropped by means of vibration dropping at a dripper temperature of 150° C. and a vibration frequency of 150 Hz under a dropping pressure of 2 Bar; the dropping rate was matched with the melting rate in Step (1); and,
  • (3) Condensation step: the medicine drops were cooled with a cooling gas rapidly to solidify and obtained uncoated drop pills having a particle size of 2 mm; the temperature of the cooling gas was at −100° C.;
  • (4) Drying step: the resultant drop pills were dried in a fluidized drying device at 50° C. for 2 hours to give dried uncoated drop pills; and,
  • (5) Coating step: the dried uncoated drop pills were coated in a fluidized bed to coat at 35° C. to give coated drop pills; the ratio of the coating material of CAP to the uncoated drop pills was 1:25 by weight; the concentration of coating solution was 25 wt %.
    • QMDP Preparative Example 9
  • The following materials were prepared: 90 g of the API of QMDP powder and 270 g of PEG-1000. The QMDP was prepared by the following method:
  • The API of QMDP powder was added with water and stirred at 30° C. for 10 min or longer to give a pre-mixed material.
  • (1) Material melting step: the pre-mixed material and PEG-1000 were loaded into a homogenizer to homogenize at 2500 rpm for 100 min and molten homogenously at 6000 rpm for 20 min to give a molten medicine liquid; during the melting process, the temperature of the material was kept at 100° C.;
  • (2) Dropping step: the molten medicine liquid was delivered to a dripper and dropped by means of vibration dropping at a dripper temperature of 70° C., a vibration frequency of 100 Hz under a dropping pressure of 1.0 Bar, an acceleration speed of 1G and a dropping rate of 10 Kg/h, which was matched with the melting rate in Step (1);
  • (3) Condensation step: the medicine drops were cooled with a cooling gas rapidly to solidify and obtained uncoated drop pill having a particle size of 2 mm; the temperature of the cooling gas was at −80° C.;
  • (4) Drying step: the resultant drop pills were dried by a gradient-rising temperature drying method, fluidized at −20° C., dried at 15° C. for 10 min, at 35° C. for 10 min and at 55° C. for 30 min to give dried uncoated drop pills; and,
  • (5) Coating step: the dried uncoated drop pills were coated in a fluidized bed at 40° C. to give coated drop pills; the ratio of the coating material of Opadry to the uncoated drop pill was 1:25 by weight; the concentration of coating solution was 20 wt %.
    • QMDP Preparative Example 10
  • The following materials were prepared: 105 g of the API of QMDP powder and 35 g of a PEG-4000 and PEG-6000 (1:1) mixture. The QMDP was prepared by the following method:
  • The API of QMDP powder was added with water and stirred at 80° C. for 10 min or longer to give a pre-mixed material.
  • (1) Material melting step: the pre-mixed material and the PEG-4000 and PEG-6000 (1:1) mixture were loaded into a homogenizer to homogenize at 2500 rpm for 100 min and molten homogenously at 6000 rpm for 80 min to give a molten medicine liquid; during the melting process, the temperature of the material was kept at 80° C.;
  • (2) Dropping step: the molten medicine liquid was delivered to a dripper and dropped by means of vibration dropping at a dripper temperature of 100° C., a vibration frequency of 200 Hz under a dropping pressure of 3.0 Bar, an acceleration speed of 20G and a dropping rate of 40 Kg/h, which was matched with the melting rate in Step (1);
  • (3) Condensation step: the medicine drops were cooled with a cooling gas rapidly to solidify and obtained uncoated drop pills having a particle size of 2 mm; the temperature of the cooling gas was at −120° C.;
  • (4) Drying step: the resultant drop pills were dried by a gradient-rising temperature drying method, fluidized at 30° C., dried at 35° C. for 120 min, at 55° C. for 60 min and at 100° C. for 60 min to give dried uncoated drop pills; and,
  • (5) Coating step: the dried uncoated drop pills were coated in a fluidized bed at 35° C. to give coated drop pills; the ratio of the coating material of methyl acrylate to the uncoated drop pills was 1:25 by weight; the concentration of coating solution was 5 wt %.
  • As found in the study by the inventors, compared with the current Qishenyiqi drop pills, the Qishenyiqi micro drop pills prepared by the methods disclosed in QMDP PREPARATIVE EXAMPLES 1˜10 had the same merits listed in Table 2.
    • Example 3 Salvia Militiorrhiza Micro Drop Pill (SMDP) SMDP Preparative Example 1
  • 600 g of the Salvia Militiorrhiza extract was added with water (60 g) and 1500 g of PEG-6000, charged into a melting tank and totally molten and mixed to give a molten medicine liquid by heating to 90° C. The molten medicine liquid was delivered under pressure to a dripper and dropped by means of vibration dropping at a dripper temperature of 80° C. and a vibration frequency of 20 Hz, the dripper was heated and preserved by infrared ray. The medicine drops were cooled with low-temperature nitrogen and the cooling temperature was −10° C. The drop pills were dried and drug-loading coated in a fluidized bed, screened, regulated and packaged to give the final product.
  • Wherein, the Salvia Militiorrhiza extract can either be prepared by the conventional methods or commercially available.
    • SMDP Preparative Example 2
  • 600 g of the Salvia Militiorrhiza extract was added with water (60 g) and 600 g of PEG-6000, charged into a melting tank and totally molten and mixed to give a molten medicine liquid by heating to 90° C.˜100° C. The molten medicine liquid was delivered under pressure to a dripper and dropped by means of vibration dropping at a dripper temperature of 80° C.˜100° C. and a vibration frequency of 150 Hz. The drops were cooled with low-temperature nitrogen and the cooling temperature was −140° C. The drop pills were dried with a fluidized bed at 150° C. and coated with a coating solution (18˜20 wt %), screened, regulated and packaged to give the final product.
  • Wherein, the Salvia Militiorrhiza extract can either be prepared by the conventional methods or commercially available.
    • Example 4 Huoxiangzhengqi Micro Drop Pill (HMDP) HMDP Preparative Example 1
  • 200 g of Huoxiangzhengqi extract, 1 ml of patchouli oil, 2 ml of perilla leaf oil and 600 g of PEG-6000 were charged into a melting tank and molten by heating to 65° C.−85° C. to give an uniform liquid. The vibration frequency of an electronic dripper was adjusted to 200 Hz. The temperature of the dripper was controlled at 80° C. The molten medicine liquid was flowed under pressure into the dripper and dropped from the bottom of the dripper into a cooling duct. The drops were cooled with low-temperature nitrogen to give solid drop pills. The cooling temperature was −20° C. The drop pills were dried in a fluidized state at 60° C. and coated with a coating solution (15 wt %). The drop pills were screened, regulated and packaged to obtain the final product.
  • Wherein, the Huoxiangzhengqi extract can be prepared by the methods disclosed in Chinese patent applications CN 100563635A and CN 1745799A and patchouli oil and perilla leaf oil were commercially available.
    • HMDP Preparative Example 2
  • 200 g of Huoxiangzhengqi extract, 1 ml of patchouli oil, 2 ml of perilla leaf oil and 600 g of PEG-6000 were prepared. All of the Huoxiangzhengqi extract and 550 g of PEG-6000 was charged into 1# melting tank and molten by heating to 65˜85° C. to give a uniform liquid. 1 ml of patchouli oil, 2 ml of perilla leaf oil and 50 g of PEG-6000 were charged into 2# melting tank and molten by heating to 65˜85° C. to give a uniform liquid. The liquid in 2# melting tank was delivered to the inner layer of a double-layer dripper and the liquid in 1# melting tank was delivered to the outer layer of the double-layer dripper. The vibration frequency of the dripper was adjusted to 200 Hz. The molten medicine liquid was flowed under pressure into the dripper and dropped by means of vibration dropping at a dripper temperature of 80° C. The drops were cooled with low-temperature air to give solid drop pills. The cooling temperature was −40° C. By using the same method as HMDP PREPARATIVE EXAMPLE 1, the drop pills were dried in a fluidized state and drug-loading coated, screened, regulated and packaged to obtain the final product.
  • Wherein, the Huoxiangzhengqi extract can be prepared by the methods disclosed in Chinese patent applications CN 100563635A and CN 1745799A and the patchouli oil and perilla leaf oil were commercially available.
    • Example 5 Andrographolide Micro Drop Pill (AMDP) AMDP Preparative Example 1
  • 400 g of andrographolide, 800 g of PEG-6000 and 800 g of PEG-4000 were prepared. The PEG-6000 and PEG-4000 were charged into a melting tank and pre-molten by heating to 70˜80° C., into which the andrographolide was added and mixed to give a uniform liquid. The vibration frequency of a pneumatic dripper was adjusted to 30 Hz. The temperature of the dripper was controlled at 80° C. The molten medicine liquid was flowed under pressure into the dripper and dropped from the bottom of the dripper into a cooling duct. The drops were cooled with low-temperature nitrogen to give solid drop pills. The cooling temperature was −20° C. The drop pills were dried in a fluidized state and coated with a coating solution (25 wt %). The drop pills were screened, regulated and packaged to obtain the final product.
    • AMDP Preparative Example 2
  • 400 g of andrographolide and 400 g of starch were prepared. The starch was charged into a melting tank and pre-molten by heating to 70˜80° C., into which the andrographolide was added and mixed to give a uniform liquid. The vibration frequency of a pneumatic dripper was adjusted to 30 Hz. The temperature of the dripper was controlled at 80° C. The molten medicine liquid was flowed under pressure into the dripper and dropped from the bottom of the dripper into a cooling duct. The drops were cooled with low-temperature nitrogen to give solid drop pills. The cooling temperature was −20° C. The drop pills were dried in a fluidized state and drug loading coated. The drop pills were screened, regulated and packaged to obtain the final product with a particle size of drop pill of 0.5 mm˜1 mm.
    • AMDP Preparative Example 3
  • 1200 g of andrographolide and 400 g of carboxymethyl cellulose (CMC) were prepared. The CMC was charged into a melting tank and pre-molten by heating to 90˜100° C., into which the andrographolide was added and mixed to give a uniform liquid. The vibration frequency of a pneumatic dripper was adjusted to 30 Hz. The temperature of the dripper was controlled at 80° C. The molten medicine liquid was flowed under pressure into the dripper and dropped from the bottom of the dripper into a cooling duct. The drops were cooled with low-temperature nitrogen to give solid drop pills. The cooling temperature was −20° C. The drop pills were dried in a fluidized state and drug loading coated. The drop pills were screened, regulated and packaged to obtain the final product with a particle size of drop pill of 1.5 mm˜2 mm.
  • The andrographolide was either prepared by the methods known in the prior art or commercially available.
    • Example 6 Compound Ginkgo Biloba Micro Drop Pill (CGMDP) CGMDP Preparative Example 1
  • 600 g of Salvia Militiorrhiza and Ginkgo Biloba extract and 2000 g of PEG-6000 were prepared. The PEG-6000 was charged into a melting tank and pre-molten by heating to 90° C., into which the Salvia Militiorrhiza and gingko extract was added and mixed to give a uniform liquid. The vibration frequency of a pneumatic dripper was adjusted to 50 Hz. The temperature of the dripper was controlled at 80° C. The molten medicine liquid was flowed under pressure into the dripper and dropped from the bottom of the dripper into a cooling duct. The drops were cooled with low-temperature inert gas to give solid drop pills. The cooling temperature was −20° C. The drop pills were dried in a fluidized state at 75° C. and drug loading coated to obtain drop pills with a particle size of 1.0 mm˜2.0 mm. The drop pills were loaded into capsules, and 100% of the capsules were on-line checkweighed with a capsule checkweigher, packaged to give the final product.
  • Wherein, the Salvia Militiorrhiza and Ginkgo Biloba extract was prepared by the method of Chinese patent CN 1872099B.
  • During the process of dropping, the formation of drop pills was measured visually by using a stroboscopic illumination to perform real-time monitoring and adjustment. In order to improve the uniformity and roundness of the drop pills, the step of screening and regulating could be added.
    • CGMDP Preparative Example 2
  • 600 g of Salvia Militiorrhiza and Ginkgo Biloba extract and 2000 g of PEG-6000 were prepared. The PEG-6000 was charged into a melting tank and pre-molten by heating to 90° C., into which the Salvia Militiorrhiza and Ginkgo Biloba extract was added and mixed to give a uniform liquid. The vibration frequency of a pneumatic dripper was adjusted to 50 Hz. The temperature of the dripper was controlled at 80° C. The molten medicine liquid was flowed under pressure into the dripper and dropped from the bottom of the dripper into a cooling duct. The drops were cooled with low-temperature inert gas to give solid drop pills. The cooling temperature was −20° C. The drop pills were dried in a fluidized state at 75° C. and drug loading coated to obtain drop pills with a particle size of 1.0 mm˜2.0 mm. The drop pills were loaded into capsules, and 100% of the capsules were on-line checkweighed with a capsule checkweigher, packaged to give the final product.
  • Wherein, the Salvia Militiorrhiza and Ginkgo Biloba extract was prepared by the method of Chinese patent CN 101015527B.
  • During the process of dropping, the formation of drop pills was measured visually by using a stroboscopic illumination to perform real-time monitoring and adjustment. In order to improve the uniformity and roundness of the drop pills, the step of screening and regulating could be added.
    • Example 7 Guanxindanshen Micro Drop Pill (GMDP)
  • 600 g of Salvia Militiorrhiza and Panax Notoginseng extract, 5 g of volatile oil from Lignum Dalbergiae Odoriferae and 2000 g of PEG-6000 were prepared. The PEG-6000 was charged into a melting tank and pre-molten by heating to 90° C., into which the Salvia Militiorrhiza and Panax Notoginseng extract and the volatile oil from Lignum Dalbergiae Odoriferae were added and mixed to give a uniform liquid. The vibration frequency of a pneumatic dripper was adjusted to 50 Hz. The temperature of the dripper was controlled at 80° C. The molten medicine liquid was flowed under pressure into the dripper and dropped from the bottom of the dripper into a cooling duct. The drops were cooled with low-temperature inert gas to give solid drop pills. The cooling temperature was −20° C. The drop pills were dried in a fluidized state at 75° C. and drug loading coated to obtain drop pills with a particle size of 1.0 mm˜2.0 mm. The drop pills were loaded into capsules, and 100% of the capsules were on-line checkweighed with a capsule checkweigher, packaged to give the final product.
  • Wherein, the Salvia Militiorrhiza and Panax Notoginseng extract and volatile oil from Lignum Dalbergiae Odoriferae were commercially available. Also, the Salvia Militiorrhiza and Panax Notoginseng extract can be prepared by the method for preparing the Salvia Militiorrhiza and Panax Notoginseng extract in the preparation of the CSMDP or QMDP.
  • During the process of dropping, the formation of drop pills was measured visually by using a stroboscopic illumination to perform real-time monitoring and adjustment. In order to improve the uniformity and roundness of the drop pills, the step of screening and regulating could be added.
    • Example 8 Xuesaitong Micro Drop Pill (XMDP)
  • 400 g of Panax Notoginseng saponins (PNS) and 400 g of starch were prepared. The starch was charged into a melting tank and pre-molten by heating to 70˜80° C., into which the PNS was added and mixed to give a uniform liquid. The vibration frequency of a pneumatic dripper was adjusted to 30 Hz. The temperature of the dripper was controlled at 80° C. The molten medicine liquid was flowed under pressure into the dripper that was heat-insulated by a steam jacket and dropped from the bottom of the dripper into a cooling duct. The drops were cooled with low-temperature nitrogen to give solid drop pills. The cooling temperature was −20° C. The drop pills were dried in a fluidized state, drug loading coated and packaged to obtain drop pills with a particle size of 0.5 mm˜1 mm.
  • As found in the study by the inventors, compared with the current drop pill, the micro drop pills prepared by the methods disclosed in EXAMPLES 3˜8 had the same merits listed in Table 2.

Claims (19)

What is claimed is:
1. A preparation method for a Chinese medicine micro drop pill comprising the following steps:
(1) a material melting step comprising heat melting a medicine and a drop pill matrix at 40° C.-120° C. and homogenizing to obtain a homogenized molten medicine liquid, and the ratio of the medicine to the drop pill matrix is 1:3-5:1 by weight;
(2) a dropping step comprising delivering the molten medicine liquid under pressure to a dripper, and acquiring medicine drops of the molten medicine liquid by vibration dropping at a vibration frequency for dropping of 20-300 Hz under a dropping pressure of 0.5-4.0 Bar, a temperature of the dripper of 40° C.-200° C. and a viscosity of the molten medicine liquid of 300-1500 cp;
(3) a condensation step comprising cooling the medicine drops with a cooling gas to obtain micro drop pills having a particle size of 0.2 mm-2.5 mm, wherein the temperature of the cooling gas is −40° C. to −200° C. to produce low temperature micro drop pills; and
(4) a drying step comprising drying the low-temperature micro drop pills from Step (3) on a fluidized-bed to obtain uncoated micro drop pills with a water content of 3%-7%, using a gradient-rising temperature drying method comprising first fluidizing at −20-30° C., then sequentially drying at 15-35° C. for 10-120 minutes (min), 35-55° C. for 10-60 min, and 55-100° C. for 0-60 min.
2. The preparation method according to claim 1, wherein in Step (1), the drop pill matrix comprises PEGs, sorbitol, xylitol, lactitol, maltose, starch, methylcellulose, sodium carboxymethyl cellulose, hydroxypropyl methylcellulose, arabic gum, alginic acid, dextrin, cyclodextrin, agar, lactose or any combination thereof.
3. The preparation method according to claim 1, wherein in Step (2), the dripper is at a temperature of 60-120° C.; the vibration frequency for dropping is 50-300 Hz; and the vibration dropping comprises magnetic/electronic vibration or pneumatic vibration; and, the molten medicine liquid has a viscosity of 500-1000 cp.
4. The preparation method according to claim 1, wherein:
(1) the material melting step comprises placing the medicine and the drop pill matrix into a homogenizer, mixing homogenously at 1000-5000 rpm for 1-200 min, then melting homogenously at 3000-10000 rpm for 1-100 min, wherein during melting the temperature is kept at 60-100° C. to obtain the molten medicine liquid, and wherein the ratio of the medicine to the micro drop pill matrix is 1:3-5:1 by weight;
(2) the dropping step comprises delivering the molten medicine liquid under pressure to the dripper, and acquiring medicine drops from the dripper using vibration dropping at a vibration frequency for dropping of 50-300 Hz under a dropping pressure of 0.5-4.0 Bar, wherein the dripper is at a temperature of 40° C.-200° C., and wherein a dropping rate is matched with melting rate of Step (1); and
(3) the condensation step comprises cooling the medicine drops with a cooling gas rapidly to solidify, and obtaining solid drop pills having a particle size of 0.2 mm-2.5 mm, wherein the temperature of the cooling gas is −60° C. to −150° C.;
(4) a drying step comprises drying the low-temperature micro drop pills from Step (3) on a fluidized-bed to obtain uncoated micro drop pills with a water content of 3%-7%, wherein a gradient-rising temperature drying method is used, and wherein the gradient-rising temperature drying method comprises first fluidizing at −20-30° C., and then sequentially drying at 15-35° C. for 10-120 min, 35-55° C. for 10-60 min, and 55-100° C. for 0-60 min.
5. The preparation method according to claim 4, wherein in Step (1), the ratio of the medicine to the drop pill matrix is 1:2.3-3:1 by weight, and wherein Step (1) comprises mixing homogeneously at 3000-5000 rpm for 10-60 min, then melting homogeneously at 4000-9000 rpm for 5-30 min, and wherein during the melting process, the temperature is kept at 70° C.-90° C.
6. The preparation method according to claim 4, wherein in Step (1), the ratio of the medicine to the drop pill matrix is 1:(1-3) by weight, and wherein Step (1) comprises mixing homogeneously at 3000-4000 rpm for 10-30 min, then melting homogeneously at 4000-6000 rpm for 6-30 min, and wherein during the melting process, the temperature is kept at 75° C.-85° C.
7. The preparation method according to claim 4, wherein in Step (2), the temperature of the dripper is at 70° C.-100° C., the vibration frequency is at 90-200 Hz, and the dropping pressure is at 1.0-3.0 Bar.
8. The preparation method according to claim 4, wherein in Step (2), the dropping rate is 10-40 Kg/h.
9. The preparation method according to claim 1, wherein the method additionally comprises:
(5) a coating step comprising coating the uncoated drop pills obtained from Step (4) in a state of fluidization, wherein the coating liquid is at a concentration of 15 wt %-25 wt %; and the ratio of coating material to the uncoated drop pill is 1:50-1:25 by weight.
10. The preparation method according to claim 1, wherein in Step (1), the medicine and the drop pill matrix are added with water, and then the medicine, the drop pill matrix and the water are melted with heat.
11. The preparation method according to claim 1, wherein the gradient-rising temperature drying method is: fluidizing at 0-20° C., drying at 25° C. for 60 min, drying at 45° C. for 30 min, and drying at 55° C. for 0-30 min.
12. The preparation method according to claim 4, wherein the gradient-rising temperature drying method is: fluidizing at 0-20° C., drying at 25° C. for 60 min, drying at 45° C. for 30 min, and drying at 55° C. for 0-30 min.
13. The preparation method according to claim 1, wherein, micro drop pill weight obtained at step (3) is 3 mg-5 mg.
14. The preparation method according to claim 9, wherein the coating material comprises a shellac, CAP, methyl acrylate, or methyl methacrylate.
15. The preparation method according to claim 1, wherein the Chinese medicine micro drop pill is a Compound Salvia Militiorrhiza micro drop pill (CSMDP), a Qishenyiqi micro drop pill (QMDP), a Salvia Militiorrhiza micro drop pill (SMDP), a Huoxiangzhengqi micro drop pill (HMDP), a Andrographis Paniculata micro drop pill (AMDP), a Compound Ginkgo Biloba micro drop pill (CGMDP), a Guanxindanshen micro drop pill (GMDP) or a Xuesaitong micro drop pill (XMDP).
16. A formulation of a micro drop pill, wherein the micro drop pill has a ratio of medicine to drop pill matrix of 1:3-5:1 by weight, a particle size of 0.2 mm-2.5 mm, the micro drop bill is prepared by the method of claim 1, and wherein the micro drop pill has no residual coolant.
17. The formulation of the micro drop pill according to claim 16, wherein the particle size is 0.2 mm-2 mm.
18. The formulation of the micro drop pill according to claim 16, wherein the formulation of micro drop pill is a Compound Salvia Militiorrhiza micro drop pill (CSMDP), the micro drop pill is prepared by the API of Compound Salvia Militiorrhiza and the drop pill matrix in a ratio of 1:3-5:1 by weight, the particle size of the Compound Salvia Militiorrhiza micro drop pill is 0.2 mm-2.5 mm, the API of Compound Salvia Militiorrhiza is prepared by the following crude drugs by weight parts: Salvia Militiorrhiza 75.0-90.0 parts, Panax Notoginseng 10.0-25.0 parts and borneol 0.1-4.0 parts.
19. The formulation of micro drop pill according to claim 16, wherein the formulation of micro drop pill is a Qishenyiqi micro drop pill (QMDP), characterized in that the micro drop pill is prepared by the API of Qishenyiqi and the drop pill matrix in a ratio of 1:3-5:1 by weight, the particle size of the Qishenyiqi micro drop pill is 0.2 mm-2.5 mm, the API is prepared by the following crude drugs by weight parts: Astragalus membranaceus 100-200 parts, Salvia Militiorrhiza 50-100 parts, Panax Notoginseng 10-20 parts and volatile oil from Lignum Dalbergiae Odoriferae 0.5-2 parts.
US16/422,857 2013-07-11 2019-05-24 Formulation of a micro drop pill and the preparation method thereof Active US11013694B2 (en)

Priority Applications (1)

Application Number Priority Date Filing Date Title
US16/422,857 US11013694B2 (en) 2013-07-11 2019-05-24 Formulation of a micro drop pill and the preparation method thereof

Applications Claiming Priority (11)

Application Number Priority Date Filing Date Title
CN201310291465.2A CN104274416B (en) 2013-07-11 2013-07-11 A kind of method for vibrating dripping droplet ball
CN201310290966.9A CN104274319A (en) 2013-07-11 2013-07-11 Method for dropping drop pills by vibration
CN201310290967.3A CN104274517B (en) 2013-07-11 2013-07-11 Vibratory drilling method prepares stilbene ginseng QI invigorating droplet ball
CN201310290967.3 2013-07-11
CN201310290968.8 2013-07-11
CN201310290968 2013-07-11
CN201310291465.2 2013-07-11
CN201310290966.9 2013-07-11
PCT/CN2014/082104 WO2015003661A1 (en) 2013-07-11 2014-07-11 Preparation method for traditional chinese medicine micro drop pill and traditional chinese medicine micro drop pill prepared by using the method
US201614903896A 2016-01-08 2016-01-08
US16/422,857 US11013694B2 (en) 2013-07-11 2019-05-24 Formulation of a micro drop pill and the preparation method thereof

Related Parent Applications (2)

Application Number Title Priority Date Filing Date
PCT/CN2014/082104 Continuation WO2015003661A1 (en) 2013-07-11 2014-07-11 Preparation method for traditional chinese medicine micro drop pill and traditional chinese medicine micro drop pill prepared by using the method
US14/903,896 Continuation US20160151293A1 (en) 2013-07-11 2014-07-11 Formulation of a micro drop pill and the preparation method thereof

Publications (2)

Publication Number Publication Date
US20190274962A1 true US20190274962A1 (en) 2019-09-12
US11013694B2 US11013694B2 (en) 2021-05-25

Family

ID=52279365

Family Applications (2)

Application Number Title Priority Date Filing Date
US14/903,896 Abandoned US20160151293A1 (en) 2013-07-11 2014-07-11 Formulation of a micro drop pill and the preparation method thereof
US16/422,857 Active US11013694B2 (en) 2013-07-11 2019-05-24 Formulation of a micro drop pill and the preparation method thereof

Family Applications Before (1)

Application Number Title Priority Date Filing Date
US14/903,896 Abandoned US20160151293A1 (en) 2013-07-11 2014-07-11 Formulation of a micro drop pill and the preparation method thereof

Country Status (16)

Country Link
US (2) US20160151293A1 (en)
EP (1) EP3020395B1 (en)
JP (1) JP6371841B2 (en)
KR (1) KR102342819B1 (en)
AU (1) AU2014289765B2 (en)
CA (1) CA2916423C (en)
DK (1) DK3020395T3 (en)
EA (1) EA034240B1 (en)
ES (1) ES2869918T3 (en)
GE (1) GEP20186901B (en)
HK (1) HK1221156A1 (en)
HU (1) HUE054609T2 (en)
MX (1) MX2015017651A (en)
TW (1) TWI653991B (en)
UA (1) UA119750C2 (en)
WO (1) WO2015003661A1 (en)

Cited By (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
CN113218480A (en) * 2020-04-14 2021-08-06 浙江大学 Characterization method of pill weight of dropping pills

Families Citing this family (3)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
CN104418744B (en) 2013-08-29 2017-03-01 天士力制药集团股份有限公司 A kind of new salvianolic acid compound T, Preparation Method And The Use
CN107782798B (en) * 2016-08-24 2021-09-21 天士力医药集团股份有限公司 Method for detecting qi-tonifying astragalus-ginseng dropping pills by using dual-wavelength UPLC
CN106344410B (en) * 2016-09-21 2023-03-14 吉林省农业机械研究院 Traditional Chinese medicine decocting system with secondary medicine adding device and traditional Chinese medicine decocting method

Citations (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
CN101279220A (en) * 2007-12-28 2008-10-08 天津天士力制药股份有限公司 Method for preparing dropping pill using cool air and equipment using the method

Family Cites Families (90)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US3436837A (en) 1963-08-13 1969-04-08 Us Army Fluidized bed freeze drying
GB8509035D0 (en) 1985-04-09 1985-05-15 Pepper D S Preparation of porous bodies
FR2602986A2 (en) 1986-04-10 1988-02-26 Tortochot Gerard Device for cleaning waste disposal, ventilation or sewage pipes
JPS63277616A (en) 1987-05-09 1988-11-15 Taisho Pharmaceut Co Ltd Production of flavoring oral pharmaceutical
DE4201178C2 (en) 1992-01-17 1995-12-07 Alfatec Pharma Gmbh Process for the production of soft gelatin capsules by a dropping process
US6080429A (en) 1993-10-25 2000-06-27 Genentech, Inc. Method for drying microspheres
JP2002104958A (en) 2000-09-29 2002-04-10 Sumitomo Chem Co Ltd Lipophilic vitamin preparation
CN2448361Y (en) 2000-11-02 2001-09-19 傅崇东 Miniature fluidized bed medicine coating machine
UA80393C2 (en) 2000-12-07 2007-09-25 Алтана Фарма Аг Pharmaceutical preparation comprising an pde inhibitor dispersed on a matrix
US8486464B2 (en) 2000-12-22 2013-07-16 Tasly Pharmaceutical Group Co. Ltd. Herbal composition for angina pectoris, method to prepare same and uses thereof
HUP0303906A3 (en) 2000-12-22 2005-05-30 Cardionat Inc Whitestone Herbal composition for angina pectoris, method to prepare same and uses thereof
CN2508752Y (en) 2001-10-10 2002-09-04 王明川 Steady temperature and constant pressure full automatic machine for making chinese herb medicine pills
JP4429590B2 (en) 2002-02-08 2010-03-10 株式会社協和ウェルネス Ubiquinone-containing water-soluble composition
CN1470255A (en) 2002-07-22 2004-01-28 王智民 Preparation extracted from the root of red-rooted solvia and pseudo-ginseng and its compound preparation and medical use
CN1267111C (en) 2002-12-23 2006-08-02 北京采瑞医药有限公司 Compound red sage drip pill for treating cardiac and cerebral vascular diseases and its prepn process
US20050037094A1 (en) * 2003-07-31 2005-02-17 Xijun Yan Composition for heart disease, its active ingredients, method to prepare same and uses thereof
CN100404040C (en) 2003-09-19 2008-07-23 天津天士力制药股份有限公司 Medicinal composition for treating cardiopathy and its preparation method and use
CN100339085C (en) 2003-09-23 2007-09-26 天津天士力制药股份有限公司 Combination of Chinese traditional medicine for curing cardiovascular and cerebrovascular diseases
CN100404035C (en) 2003-09-23 2008-07-23 天津天士力制药股份有限公司 Combination of Chinese traditional medicine for curing cardiovascular diseases and cerebrovascular disease
CN1297288C (en) 2003-11-19 2007-01-31 王锦刚 Medicine for treating cardiovascular disease, and its prepn. method
CN100563673C (en) * 2003-12-11 2009-12-02 天津天士力制药股份有限公司 Chinese medicine preparation of treatment angina pectoris and preparation method thereof
CN100563635C (en) 2003-12-11 2009-12-02 天津天士力制药股份有限公司 A kind of ageratum drop pill
CN100450501C (en) 2004-03-17 2009-01-14 天津天士力制药股份有限公司 Chinese medicine preparation for treating cardiovascular and cerebrovascular diseases and preparing process thereof
JP2005306778A (en) * 2004-04-21 2005-11-04 Basf Ag Sustained-release formulation and method for producing the same
CN100404041C (en) 2004-06-30 2008-07-23 天津天士力制药股份有限公司 Medicinal composition for treating coronary heart disease
CN1745768B (en) * 2004-09-07 2011-03-23 天津天士力制药股份有限公司 Use of medicine containing Milkvetch Root against aspirin
CN1745769A (en) * 2004-09-07 2006-03-15 天津天士力制药股份有限公司 Use of medicine composition containing Milkvetch Root
CN100522214C (en) 2004-09-07 2009-08-05 天津天士力制药股份有限公司 Huoxiang Zhengqi drop pill an dits preparation
CN100411642C (en) 2004-10-15 2008-08-20 合肥恒星药物研究所 Medication for treating chronic hepatitis
CN1633992A (en) * 2004-11-12 2005-07-06 康国忠 Pharmaceutical drop pills and its preparation method
US7727555B2 (en) 2005-03-02 2010-06-01 Boston Scientific Scimed, Inc. Particles
US9161918B2 (en) * 2005-05-02 2015-10-20 Adare Pharmaceuticals, Inc. Timed, pulsatile release systems
CN2794513Y (en) 2005-05-11 2006-07-12 闵金杆 Dripping pill machine
CN1872099B (en) 2005-06-01 2010-09-29 天津天士力制药股份有限公司 Medication for treating cardiovascular diseases, and cerebrovascular disease
CN1939406A (en) * 2005-09-26 2007-04-04 刘凤鸣 Danshen root drop pills for treating coronary heart disease and preparation thereof
EP1774971A1 (en) * 2005-10-14 2007-04-18 Advanced in Vitro Cell Technologies, S.L. Chitosan and heparin nanoparticles
CN100335897C (en) 2005-11-02 2007-09-05 中国药科大学 Quality detection method for compound prepn of red sage and notoginseng
CN100594021C (en) 2005-12-06 2010-03-17 河北工业大学 Automatic medicinal dropping pill machine
US20070128272A1 (en) 2005-12-07 2007-06-07 Zerbe Horst G Multi-vitamin and mineral supplement
CN2865683Y (en) 2006-01-06 2007-02-07 聊城万合工业制造有限公司 Whole automatic controller for drop pills machine based on PLC control
CN101015527B (en) 2006-02-08 2011-05-18 天津天士力制药股份有限公司 Dropping pills preparation
CN100512830C (en) 2006-05-17 2009-07-15 广州白云山和记黄埔中药有限公司 Pharmaceutical composition for treating senile dementia
AU2006344099B2 (en) * 2006-06-06 2013-02-28 Universidad Autonoma Metropolitana Sol-gel nanostructured titania reservoirs for use in the controlled release of drugs in the central nervous system and method of synthesis
CN101085000B (en) 2006-06-08 2012-04-18 天津天士力之骄药业有限公司 Compound red sage root freezing-dried powder injection containing salvianolic acid B and its preparation method
CN101143152B (en) 2006-09-15 2011-07-27 杨明 Dripping pill for treating digestive ulcer and medicine composition containing the same
CN200948597Y (en) 2006-09-25 2007-09-19 湖南大学 Submerged intelligent cleaning robot for large-scale condensing plant
CN100457748C (en) 2006-10-18 2009-02-04 中国医学科学院医药生物技术研究所 Novel phenolic acid compounds of tanshin polyphenolic acid N and application thereof
CN101020028B (en) 2006-11-11 2010-05-19 刘光辉 Chinese medicine for treating cardiac and cerebral vascular diseases
WO2008126720A1 (en) * 2007-04-06 2008-10-23 Senju Pharmaceutical Co., Ltd. Suspension for visualization of transparent tissue in eye
ES2963291T3 (en) 2007-04-26 2024-03-26 Sublimity Therapeutics Ltd Manufacturing of multiple mini capsules
JP5229606B2 (en) 2007-05-16 2013-07-03 株式会社リコー Toner manufacturing method and toner manufacturing apparatus
CN101439076B (en) * 2007-11-22 2012-04-18 天津天士力制药股份有限公司 Preparation method of chinese medicine granule containing dalbergia heartwood oil
CN101229099B (en) 2007-12-28 2011-06-08 天津天士力制药股份有限公司 Equipment for preparing pill using cold wind and trap cooling gas
CN201200979Y (en) 2008-06-11 2009-03-04 深圳市鑫承诺科技有限公司 Online spraying and cleaning equipment
RU2475261C2 (en) 2008-07-29 2013-02-20 Хэбэй Млин Медсин Рисерч Инститьют Ко., Лтд. APPLICATION OF TRADITIONAL CHINESE MEDICAL COMPOSITION FOR OBTAINING MEDICATION FOR PROMOTION OF SURVIVAL OF OBTAINED FROM BONE MARROW MESENCHYMAL STEM CELLS in vivo AND THEIR DIFFERENTIATION IN CARDIOMYOCYTES
CN100554840C (en) 2008-08-11 2009-10-28 常州先锋干燥设备有限公司 Vibration fluidization drying system
CN201253349Y (en) 2008-09-25 2009-06-10 高月荣 Ultrasonic atomization method medicine micro-spheres preparation method
CN101711792B8 (en) 2008-10-06 2020-12-22 天士力医药集团股份有限公司 Dripping pill for treating coronary heart disease and preparation method thereof
CN101744722B (en) 2008-12-03 2013-09-11 天士力制药集团股份有限公司 Dripping pill production line
US20100151036A1 (en) * 2008-12-16 2010-06-17 Bin Wu Multiphase drug delivery system
CN101757475A (en) 2008-12-25 2010-06-30 天津药物研究院 Method for preparing fresh snow preparation
CN101518495B (en) * 2009-03-26 2011-12-28 天津大学 Vibration crushing type pill dropping machine
US20120041062A1 (en) 2009-03-30 2012-02-16 Tianjin Tasly Pharmaceutical Co., Ltd. Compound of salvianolic acid l, preparation method and use thereof
CN101579449A (en) * 2009-05-18 2009-11-18 广州星群(药业)股份有限公司 Method for preparing oleum viticis negundo dripping pills
CN101584743A (en) 2009-06-02 2009-11-25 耿福能 Method for preparing Chinese traditional medicinal compound salvia miltiorrhiza preparation for curing cardiovascular and cerebrovascular diseases
CN101612195A (en) 2009-07-17 2009-12-30 江西中医学院 A kind of polynary medicine-releasing system that contains Radix Salviae Miltiorrhizae and Radix Notoginseng
CN102048967A (en) 2009-11-05 2011-05-11 天津太平洋制药有限公司 Inflammation-diminishing and heat-clearing composition and preparation method thereof
TW201117839A (en) 2009-11-20 2011-06-01 Tianjin Tasly Pharmaceutical Drop pill for treating coronary heart disease and manufacture method thereof
CN102119964B (en) 2010-01-07 2016-11-23 天津天士力现代中药资源有限公司 A kind of prevention and the extract for the treatment of angina pectoris, their Preparation method and use
CN102119963A (en) 2010-01-07 2011-07-13 天津天士力现代中药资源有限公司 Extract for preventing and treating angina pectoris and coronary heart disease and preparation method and application thereof
CN201589495U (en) 2010-01-18 2010-09-22 山东天力干燥设备有限公司 Multifunctional intermittent drying system of freeze-spray granulation fluidized bed
US8945657B2 (en) * 2010-06-22 2015-02-03 The Coca-Cola Company Dehydrated pulp slurry and method of making
CA2807283C (en) * 2010-08-06 2019-05-14 Xijun Yan Use of salvia miltiorrhiza composition in preparing drugs for secondary prevention of coronary heart disease
CN102048707A (en) * 2010-11-29 2011-05-11 黑龙江天宏药业有限公司 Mesalazine enteric-coated tablet and preparation method thereof
CN102552256A (en) * 2010-12-23 2012-07-11 丽珠医药集团股份有限公司 Ilaprazole enteric capsule and preparation method thereof
CN102078259A (en) 2010-12-29 2011-06-01 天津大学 Equipment and method for preparing uniform dripping pills
CN102178605B (en) 2011-03-09 2014-03-26 天津大学 Traditional Chinese medicine cataplasma forming device with automatic detection function
ES2688591T3 (en) 2011-03-28 2018-11-05 Ablynx N.V. Method for producing solid formulations comprising individual variable domains of immunoglobulin
CN202027925U (en) 2011-03-29 2011-11-09 中国中医科学院中药研究所 Fully-automatic pill dripping machine with function of online detection
JP2012229173A (en) * 2011-04-26 2012-11-22 Ogawa & Co Ltd Vascular endothelial function ameliorating agent
CN102908355B (en) 2011-08-04 2014-06-04 中国科学院上海药物研究所 Medicinal composition and application thereof
CN102526446B (en) 2012-01-13 2013-11-06 张居运 Traditional Chinese medicine composition for treating coronary heart disease and method for preparing medicated wine by utilizing same
CN102526186A (en) 2012-01-17 2012-07-04 中国中医科学院广安门医院 Medicinal composition for preventing and treating cardiovascular diseases and application thereof
CN102988476A (en) * 2012-08-23 2013-03-27 江苏苏南药业实业有限公司 Method for preparing compound red-rooted salvia root dropping pills
CN204147279U (en) 2013-07-11 2015-02-11 天士力制药集团股份有限公司 Air cooling dripping pill production line
EP3020408B1 (en) 2013-07-11 2022-01-12 Tasly Pharmaceutical Group Co., Ltd. Traditional chinese medicine composition, and preparation and application thereof
USRE49050E1 (en) 2013-07-11 2022-04-26 Tasly Pharmaceutical Group Co., Ltd. Traditional Chinese medicine composition, and preparation and application thereof
US10300030B2 (en) 2013-08-29 2019-05-28 Tasly Pharmaceutical Group Co., Ltd. Traditional Chinese medicine composition
CN104418744B (en) 2013-08-29 2017-03-01 天士力制药集团股份有限公司 A kind of new salvianolic acid compound T, Preparation Method And The Use
CN204170103U (en) 2014-07-11 2015-02-25 天士力制药集团股份有限公司 Air cooling dripping pill production line

Patent Citations (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
CN101279220A (en) * 2007-12-28 2008-10-08 天津天士力制药股份有限公司 Method for preparing dropping pill using cool air and equipment using the method

Cited By (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
CN113218480A (en) * 2020-04-14 2021-08-06 浙江大学 Characterization method of pill weight of dropping pills

Also Published As

Publication number Publication date
WO2015003661A1 (en) 2015-01-15
AU2014289765B2 (en) 2019-05-09
JP6371841B2 (en) 2018-08-08
GEP20186901B (en) 2018-10-10
EP3020395A4 (en) 2016-12-07
US11013694B2 (en) 2021-05-25
UA119750C2 (en) 2019-08-12
US20160151293A1 (en) 2016-06-02
TWI653991B (en) 2019-03-21
EP3020395B1 (en) 2021-03-03
HK1221156A1 (en) 2017-05-26
KR20160028460A (en) 2016-03-11
CA2916423A1 (en) 2015-01-15
EA034240B1 (en) 2020-01-21
HUE054609T2 (en) 2021-09-28
MX2015017651A (en) 2016-11-14
DK3020395T3 (en) 2021-05-25
ES2869918T3 (en) 2021-10-26
EA201690209A1 (en) 2016-08-31
EP3020395A1 (en) 2016-05-18
JP2016528200A (en) 2016-09-15
TW201536355A (en) 2015-10-01
KR102342819B1 (en) 2021-12-22
AU2014289765A1 (en) 2016-01-21
CA2916423C (en) 2021-10-26

Similar Documents

Publication Publication Date Title
US11013694B2 (en) Formulation of a micro drop pill and the preparation method thereof
JP7090674B2 (en) Chinese herbal medicine compositions, their formulations and uses
USRE49050E1 (en) Traditional Chinese medicine composition, and preparation and application thereof
CN104274519B (en) Vibratory drilling method prepares compound danshen dripping pills
US20160136224A1 (en) Method for preparing a camellia nitidissima chi lipid-lowering and hypoglycemic agent
CN103520357B (en) Eight-gem pill (pellet) for tonifying vitality and benefiting blood
Huang et al. Metoprolol tartrate sustained-release binary matrix microspheres for oral administration produced by novel ultra-fine particle processing system
CN107982237B (en) A kind of Betapace and preparation method thereof
CN109010312A (en) A kind of preparation method of sustained-release theophylline preparation
CN101019837B (en) Ginnone ester dispersing table and its preparation method
CN109513013A (en) A kind of placebo of folium ginkgo dripping pill and preparation method thereof
CN108186563A (en) Dilantin sodium slow-release suspension and preparation method thereof
CN117338736A (en) Pharmaceutical composition, tanshinone IIA sodium sulfonate tablet, and preparation method and application thereof
CN104619322B (en) Anticancer pharmaceutical composition and its production and use
CN103816529A (en) Pharmaceutical composition for treating various serious diseases and preparation and use thereof
CN102274202B (en) Daidzein nanocrystal immediate-release capsule and preparation process thereof

Legal Events

Date Code Title Description
FEPP Fee payment procedure

Free format text: ENTITY STATUS SET TO UNDISCOUNTED (ORIGINAL EVENT CODE: BIG.); ENTITY STATUS OF PATENT OWNER: LARGE ENTITY

AS Assignment

Owner name: TASLY PHARMACEUTICAL GROUP CO., LTD., CHINA

Free format text: ASSIGNMENT OF ASSIGNORS INTEREST;ASSIGNORS:YAN, XIJUN;WU, NAIFENG;YAN, KAIJING;AND OTHERS;REEL/FRAME:049307/0939

Effective date: 20160122

STPP Information on status: patent application and granting procedure in general

Free format text: NON FINAL ACTION MAILED

STPP Information on status: patent application and granting procedure in general

Free format text: RESPONSE TO NON-FINAL OFFICE ACTION ENTERED AND FORWARDED TO EXAMINER

STPP Information on status: patent application and granting procedure in general

Free format text: DOCKETED NEW CASE - READY FOR EXAMINATION

STPP Information on status: patent application and granting procedure in general

Free format text: RESPONSE TO NON-FINAL OFFICE ACTION ENTERED AND FORWARDED TO EXAMINER

STPP Information on status: patent application and granting procedure in general

Free format text: NOTICE OF ALLOWANCE MAILED -- APPLICATION RECEIVED IN OFFICE OF PUBLICATIONS

STPP Information on status: patent application and granting procedure in general

Free format text: PUBLICATIONS -- ISSUE FEE PAYMENT VERIFIED

STCF Information on status: patent grant

Free format text: PATENTED CASE